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Application
OPTION A3 Print & Web Media
OPTION C6
OPTION B6
CANCER
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Count on
Benecol
programme partnerships
Client Genzyme
breakfast meetings
Talk to the
OPTION C3
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Concept check/tick meaning test, exam correct answer, solution, Food +/ more than food
Time to Change C-Change
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THE
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ACADEMY
PROJECT
CANCER Healthcare
Logo design and development
A
Client RDU
C-Change OPTION A4
Print and digital media
Concept C-Change (see, sea, C, look, view) Vision.change.direction.process
Job Description Logo Design and Development
C Client RDC
Concept Modular Based Digital
Time to Change
Compliance
WORK TYPE
OPTION A3
TimeCompliance to Change
ACADEMY
C-Change
Client Astellas
OPTION C3
CANCER Healthcare Free
Red Door Communications OPTION C2 16.08.2012
Application OPTION A2 OPTION C1 Print & Web Media
Application Print & Web Media
Date 22.02.2016
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Concept Healthcare Compliance (HCC) Compliance is in our DNA
Job Description Logo Design and Development for
Years
Red Door Communications 10.04.2013
Application Print & Web Media
Healthcare Cancer: Compliance
C-Change Job Description OPTION A1 Logo Design and Development for AstraZeneca
OPTION A6
Job Description Logo Design and Development for Count on Benecol/Cholesterol counts
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OPTION A4
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CANCERFree Time to Change
Healthcare Compliance
Years Free
OPTION C4
Job Description Logo Design and Development
Application Print & Web Media
Application Print & Web Media
Date 29.02.2016
red door unlimited www.reddoorunlimited.com
CLIENT
Logos OPTION D2
OPTION D3
DIFFICULT TO
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OPTION D6
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Red Door Communications 08.11.2012
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Client RDC
Concept Reaching out and helping the hard to reach
Job Description Logo Design and Development for ‘Difficult to Reach’
OPTION A1
Red Door Communications 13.09.2012
Application Print & Web Media
OPTION A2
OPTION B
Concept Connections, health
Job Description Logo Design and Development for Chemia - connected in health
FAMILIAL
EVERYTHING
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HYPERCHO LESTEROLEMIA
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OPTION D3 OPTION A4
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FAMILY OPTION A1
Concept Familial Hypercholesterolemia
OPTION A5
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Job Description Logo Design and Development
OPTION B3
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FAMILY SEE ME
Application Print & Web Media
OPTION DateA2
20.02.2015
OPTION A3
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B
OPTION D5
A
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Client Sanofi
Client Sirukumab
CROWD
Concept
SHAPED
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Job Description Logo Design and Development
Job Description Logo Design and Development
WORK TYPEFamilial Hypercholesterolemia
Logo design and development Throat Print and digital media
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Application Print & Web Media
Application Print & Web Media
Concept CrOwd shaPeD SMART
Date 12.03.2015
Application Print & Web Media
Date 02.12.2015
red door www.reddoorunl
red door unlimited www.reddoorunlimited.com
Job Description Logo Design and Development
Application Print & Web M
CLIENT
Logos OPTION A1
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OPTION A2
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COMFORTABLE
PSORIASIS CONVERSATIONS OUT OF THE
COMFORTABLE
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OPTION B1
OPTION B2
OPTION C1
OPTION A3
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Communications Network
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OPTION A5 OPTION B2
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get comfortable conversations
HIV START PSORIASIS ACTION
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OUT OF THE ACTION GROUP SHADOWS Concept Get Comfortable Conversations
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Application Print & Web Media
Client Astellas
Communications Network PSORIASIS BETTER OUT OF THE 2017 Copenhagen Meeting rest, liquids & painkillers SHADOWS
red door unlimited www.reddoorunlimited.com
Concept Hygge (a Danish word that can be vaguely translated with cosiness)
OPTION B5 HYGIENE
Job Description Logo Design and Development for The Astellas Communications Network meeting in Copenhagen
Job Description Logo Design and Development for Psoriasis: Out of the shadows
GROUP
Power To Move
HIV
Red Door Communications 10.04.2013
Application Print & Web Media
GROUP
C
Start Getting
Job Description Hygiene Action Group Logo Design and Development for
Concept HIV: start getting personal.
02 PROJECT
WORK TYPE
Logo design and development
Print and digital media
Client RDC
Kivexa pitch
Concept Lighthouse Direction
Client Treat yourself better
Power To Move
Concept To encourage consumers to self treat cold and flu symptoms, seeking pharmacy advice
HIV:PERSONAL
PERSONAL Hygiene Action Group
PERSONAL
Red Door Unlimited 23.01.2017
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OPTION B6
ACTION
Concept Shadows, skin, positivity. Shifting out of the shadows
GETTING
Client RDC/Kivexa
OUT OF THE
Job Description Logo Design and Development
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OPTION B4
OPTION B4 HYGIENE Client RDC Novartis
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Personal
OPTION B3
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SHADOWS
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OPTIONB1 A4 OPTION
TREAT YOURSELF BETTER
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Application Print & Web Media
Job Description Logo Design and Development for ViiV Healthcare DTG/Trii LOC
POWER TO MOVE
Red Door Communication 18.02.201
Application Print & Web Media
CLIENT
Infographics
COFFEE IN THE UK 79% of consumers drink coffee (either ground or instant)1,
What is breathlessness?
COFFEE HEALTH It's reassuring to know that caffeine is one of the most heavily researched compounds in the world today and the overwhelming weight of scientific information suggests that moderate caffeine consumption of four to five cups per day is safe and may even confer some health benefits3.
A common symptom of COPD is breathlessness. Breathlessness is when you feel short of breath or have trouble breathing. This is because your lungs have to work harder than normal to inhale and exhale.
What causes breathlessness?
With COPD there are 2 common conditions that cause breathlessness:
1
Chronic bronchitis
This makes it more difficult to inhale and exhale and can leave you feeling short of breath. Normal airway
79%
2
Airway with chronic bronchitis
Emphysema
For pregnant women guidelines issued by the Food Standards Agency recommend a safe upper limit of 200mg caffeine per day from all sources4.
Normal alveoli
meaning that as a nation we consume approximately
COFFEE & HYDRATION 10 MILLION 20 MILLION 30 MILLION 40 MILLION 50 MILLION 60 MILLION 70 MILLION
70 million cups of coffee per day2.
THE UK
Alveoli with emphysema
Research has shown that the amount of caffeine consumed throughout the day in a couple of cups of coffee is no more a diuretic than water5.
Therefore evidence shows that when consumed in moderation, coffee is not in fact dehydrating and can contribute to your daily fluid intake6.
With chronic bronchitis, airways in the lungs become inflamed and narrow and produce extra mucus.
Emphysema affects the alveoli, air sacs at the end of airways. With emphysema the air sacs are damaged or destroyed and cannot be repaired. With fewer air sacs, less inhaled oxygen can reach the bloodstream. This leads to breathlessness in the later stages of COPD. Emphysema also causes the lungs to lose their springiness, which means that the lungs are not emptied each time you exhale. Eventually the lungs expand too much (hyperinflation). As a result, the lungs must work harder to breathe.
Tell your doctor if you are feeling breathless. It is important to begin treatment right away to control symptoms.
How can I stay active?
17%
25%
Coffee market is continuing to grow, with sales already increasing by 17% between 2005 and 2009 and the market is forecast to continue to grow by almost a quarter by 20142.
0.5l
1.0l
1.5l
2.0l
2.5l
In the early stages of COPD, breathlessness may be felt during activities that need extra effort. These activities may include walking or running up stairs. Everyone’s lungs weaken over time, but it happens faster in people who have COPD. As COPD worsens, everyday actions like getting dressed may cause breathlessness.
Adults 19-70 years
Males
2.5 L/day
19-70 years
Females
2.0 L/day
You may think you are too breathless to exercise, but regular exercise can actually make you feel less breathless over time.
Special cases
25%
47%
Pregnant women
2.3 L/day
Lactating women
2.7 L/day
COFFEE & CANCER In 2008, coffee shop openings actually increased by 25%.
In 2009 the six biggest chains in the UK increased their retail space by 47% according to a study from the Local Data Company1.
AT PRESENT almost half the population (47%) drink coffee in coffee shops and cafés, the majority of whom are from a younger demographic1. Coffee shops also have a much stronger appeal for women, whilst men are more likely to drink and buy coffee at work1.
Data published in BioMed Central Cancer suggests that coffee consumption may reduce total cancer incidence7.
This study builds on the World Cancer Research Fund’s advice that coffee has no significant relationship with the risk of cancer at any site7.
COFFEE & HEART HEALTH Evidence has shown that moderate coffee consumption of four to five cups a day does not significantly affect people’s risk of coronary heart disease or stroke, and instead may in fact have a protective effect9.
6 Go to physical therapy if recommended by your doctor
Walk around the house
Stay mobile and participate in activities like going for a walk
See how far you can walk in 6 minutes and try to go farther next time
Consult your doctor for advice on what you can do to relieve your symptoms.
How do I talk to my doctor about my breathlessness? If at any point you discover a new symptom or if your symptoms get worse, you should call your doctor. Keep track of when your breathlessness started and how long it lasted. Also take note of what makes you feel better or worse.
How do I treat breathlessness?
47% THE COFFEE MARKET The coffee market is therefore continually expanding, revealing the entrenched love of cafe culture, dining out and the importance of coffee shops as a place for socialising and conducting business meetings and out of office work1.
REFERENCES 1. Lorem ipsum dolor sit amet, consectetur adipiscing elit. Fusce venenatis tristique enim, at suscipit tellus lobortis at. 2. Sed commodo scelerisque nulla, ullamcorper condimentum tortor sollicitudin at.
The British Heart Foundation also states that moderate amounts of caffeine do not lead to arrhythmias, coronary heart disease or effect an individual’s blood pressure10.
REFERENCES 1. Lorem ipsum dolor sit amet, consectetur adipiscing elit. Fusce venenatis tristique enim, at suscipit tellus lobortis at. 2. Sed commodo scelerisque nulla, ullamcorper condimentum tortor sollicitudin at. 3. Nunc tincidunt ultricies aliquam. Nam sit amet feugiat turpis. Morbi eu dolor sed arcu accumsan mollis eu eu eros. 4. Mauris in nunc velit, eget tristique eros. Nulla facilisi. Sed vel justo leo, eu semper odio. 5. Lorem ipsum dolor sit amet, consectetur adipiscing elit. Fusce venenatis tristique enim, at suscipit tellus lobortis at. 6. Sed commodo scelerisque nulla, ullamcorper condimentum tortor sollicitudin at. 7. Nunc tincidunt ultricies aliquam. Nam sit amet feugiat turpis. Morbi eu dolor sed arcu accumsan mollis eu eu eros. 8. Mauris in nunc velit, eget tristique eros. Nulla facilisi. Sed vel justo leo, eu semper odio.
Breathlessness caused by COPD can be treated. It’s important to start COPD treatment when you first feel breathless as this will help control other symptoms. Quitting smoking is the best way to improve the way your lungs work. There are a number of things you could do to help your lungs and help yourself feel better:
Tips on eating and energy Eating a healthy diet is important for everyone, especially if you have COPD. The muscles used for breathing in a person with COPD may need 10 times more calories than those of a person without COPD. Here are some things you could do to get the right nutrients while maintaining a healthy weight:
Drink non-caffeinated or non-alcoholic drinks
Eat high-fiber foods like vegetables and whole grains
Consult your doctor for advice on what you can do to relieve your symptoms.
Job Number: XXX/XXX/XXXXXX Date of preparation: January 2015
PROJECT
WORK TYPE
Infographic design and development
Print and digital media
Use herbs instead of salt
Stay away from foods that cause bloating (soda or fried foods)
CLIENT
Cholesterol By Numbers*
Infographics INFLUENZA AND VACCINATION
Hepatitis C (HCV) in the UK
Cholesterol affects 3 out of 5 adults in the UK1
IN CHILDREN
FACT SHEET Flu Strikes*
HCV in numbers
HEALTH AND WELLBEING
1CASES BILLION OF FLU EACH
300,000 & 500,000
3-5 MILLION ANNUAL CASES OF SEVERE ILLNESS WORLDWIDE1
YEAR GLOBALLY1
EACH YEAR UP TO AN ESTIMATED
EACH YEAR BETWEEN
RESULTING IN
14,000
DEATHS ATTRIBUTED TO FLU IN THE UK.2
DEATHS GLOBALLY
1
*Extrapolated from estimated figures for the USA
FLU
Impact of Flu
10%
CAN LEAD TO
Young children
In England, flu* affects approximately 10% of children aged 0 –14 years in an average season3
are more likely to suffer complications and hospitalisations from flu adding substantial pressures on the NHS.4,5
Bacterial lnfection
6
Pneumonia6 Ear infection6
*defined as influenza like illness (ILI)
94%
2nd
of people over 45 years old say maintaining their heart health is “extremely important” to them
39% 39
%
Heart disease ranks second among this groups health concerns
are worried about cholesterol which is a major risk factor in the development of heart disease
CHOLESTEROL AWARENESS 29% of over 45s
Almost 45% of over 45s have no idea what their cholesterol level is
have never had a cholesterol test,
216,000
Hepatitis is a general term meaning inflammation of the liver
45%
x100
For every
8% said they weren’t currently doing anything about their cholesterol level
8%
subsequently will become ill8* * Based on a U.S kindergarten study
195
Accidental exposure to infected blood (such as needle stick injury in healthcare workers)4 Via blood transfusion before 1992 (pre blood screening)5 Baby boomers (adults born between 1945 – 1965) are five times more likely to have HCV6, as they were adults when HCV infection rates were at the highest7
50% Genotype 2/3
People of South Asian origin1
Signs and symptoms
8 household members
influenza-infected children under 3 years old,
However, there are other prevalent transmission groups in the UK, who may have been infected with HCV and some are traditionally underreported:
45% of patients in the UK with HCV are genotype 1 which is the most challenging genotype to treat: 50% of patients in the UK are genotypes 2/34
45% Genotype 1
missed school because of a flu-associated illness,
were children under 17 years of age.7
Failure to treat people currently living in the UK with HCV will cost the NHS an estimated £156 million annually2
HCV is transmitted through contact with infected blood. Stereotypically, HCV has been associated with those who share needles e.g. people who inject drugs (PWID).
Hepatitis can be caused by several mechanisms, including viral infection. Hepatitis C is caused by infection with the Hepatitis C virus (HCV) – of which there are 6 different forms (genotypes)3
rising to 40% in the 45 to 54 year old population
10 children who
243
Only 1-2% of people in the UK diagnosed with HCV will receive treatment2
What is HCV?
Data suggests for every
906
Out of the hospitalised cases reported
Almost 90% of people living with HCV remain unaware, undiagnosed and untreated2
HCV is a global public health issue. In the UK HCV is estimated to affect 216,000 adults1
parental work days were lost9
WHO IS YOUR PLUS-ONE
VS
20 -30 YEARS
People infected by HCV may not experience any symptoms for 20 – 30 years8
The signs and symptoms of HCV are often asymptomatic until the disease has progressed to liver failure6
Common symptoms include: drowsiness; headaches; nausea; and abdominal pain (focussed in the liver area)9
Consequences of HCV
Flu Symptoms Symptoms appear 1 to 4 days after the virus enters the body10
34
of women
High fever11
Muscle aches and pains11
Tiredness11
Flu Spreads
Headaches11
Cough (usually dry)11
Sore throat11
only 19% of men said they were
said they were more worried about their partner’s cholesterol than their own
In contrast,
more worried about their partner’s cholesterol than their own
>7 days -
Children, particularly those of school age, are the main transmitters of flu12
Untreated, the consequences of HCV are very serious and have a significant impact on mortality and morbidity10.
19
%
%
raised cholesterol affects
men and women over 45 equally2
One in four of those aged 45 and over already take between 3 and 6 prescription meds every day
the time that children may pass on the virus10
UP TO 2 METRES13 All children aged 2, 3 and 4 years old and children in
The Annual Flu Vaccination
school years 1&2
will be eligible for the annual vaccination programme5
47%
The optimal time to get vaccinated is from September to early November14
According to the independent advisory committee to the Department of Health, the benefits of the influenza vaccination programme for all individuals in the UK could be as many as:
Flu vaccination helps cut down flu-related missed school days by over 56%15 *
11,000 fewer hospitalisations a year16
vs not vaccinating
72% say they would prefer to lower their cholesterol through diet and exercise alone
72%
Almost a third
of people infected with HCV will go on to develop cirrhosis (scarring of the liver)11
There has been a 20% increase in deaths in the UK from chronic liver disease and cirrhosis in the under 65s between 2000 and 2009
1–2% - The number of those infected and diagnosed with HCV who receive treatment in the UK2
RANKED
7th
DID YOU KNOW…? A daily intake of 1.5 –2.4g plant stanols is proven to lower LDL cholesterol by 7 – 10% in 2 to 3 weeks
World Health Organization. Immunization, Vaccines and Biologicals. Available at: http://www.who.int/immunization/topics/influenza/en/index.html [Last accessed: May 2015] Onmedica. Flu campaign extended to four-year-olds. Available at: http://www.onmedica.com/newsArticle.aspx?id=a70a003b-04e0-432a-b016-30afeab85af2 [Last accessed: April 2015] Paget J, Balderston C, Casas, I et al. Assessing the burden of paediatric influenza in Europe: the European Paediatric Influenza Analysis (EPIA) project. Eur J Paediatr. 2010;169(8):997–1008 Heikkinen T, Booy R, Campins M et al. Should healthy children be vaccinated against influenza? A consensus report of the Summits of Independent European Vaccination Experts. Eur J Pediatr. 2006;165: 223–228 Department of Health. Annual Flu Letter 2015/16. https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/418428/Annual_flu_letter_24_03_15__FINALv3_para9.pdf Last accessed July 2015 Patient UK. Influenza. Available at: http://www.patient.co.uk/doctor/influenza [Last accessed: April 2015] Public Health England. Surveillence of influenza and other respiratory viruses in the United Kingdom: Winter 2013/14. Available at: https://www.gov.uk/government/uploads/system/uploads/attachment_data/file/325203/ Flu_annual_report_June_2014.pdf [Last accessed: April 2015] Neuzil KM, Hohlbein C, Zhu, Y. Illness among schoolchildren during influenza season: effect on school absenteeism, parental absenteeism from work, and secondary illness in families. Arch Pedi 2002;156:986-991 Heikkinen T, Silvennoinen H, Peltola V et al. Burden of influenza in children in the community. J Infect Dis. 2004; 190:1369–1373. Available at: http://www.ncbi.nlm.nih.gov/pubmed/15378427/ [Last accessed: April 2015] Centers for Disease Control and Prevention. How Flu Spreads. Available at: <http://www.cdc.gov/flu/about/disease/spread.htm> [Last accessed: April 2015] World Health Organisation. Fact Sheet No 211. Available at: http://www.who.int/mediacentre/factsheets/fs211/en/ [Last accessed: April 2015] Esposito S et al. Clinical and economic impact of influenza vaccination on healthy children aged 2-5 years. Vaccine 2006;30;24(5):629-35 World Health organization. Public health agenda for influenza 2010. Available at: http://www.who.int/influenza/resources/research/research_agenda_influenza_stream_2_limiting_spread.pdf [Last accessed July 2015] NHS Choices. Available at: http://www.nhs.uk/Livewell/winterhealth/Pages/Fluandthefluvaccine.aspx [Last accessed: April 2015] Families fighting flu. Resources. Available at http://www.familiesfightingflu.org/resources/ [Last accessed April 2015] National Health Service. Children to be offered annual flu vaccine. Available at: http://www.nhs.uk/news/2012/07July/Pages/All-children-to-be-offered-annual-flu-vaccine.aspx [Last accessed: April 2015] AstraZeneca Data on File: FLU-007-APR2015
According to the Euro Hepatitis Index, the UK ranks seventh for its capacity to handle the threat of hepatitis16
FOODS AND ACTIVITIES THAT HELP TO REDUCE CHOLESTEROL Eating cholesterol lowering functional foods that contain plant stanols or plant sterols is clinically proven to lower LDL cholesterol
Economic burden of HCV
Reducing dairy products Reducing red meats Eating more wholegrains & oats Eating more fish Eating more soya Exercise * Based on research undertaken by Redshift Research on behalf of Benecol amongst 2000 people over 45 in the UK
References: 1. Heart UK, ‘Cholesterol – The Silent Killer http://heartuk.org.uk/files/uploads/documents/HUK_memberapplicationform.pdf (Accessed 25th February 2014) 2. Townsend N, Wickramasinghe K, Bhatnagar P, Smolina K, Nichols M, Leal J, Luengo-Fernandez R, Rayner M (2012). Coronary heart disease statistics 2012 edition. British Heart Foundation: London.
May 2014
Print and digital media
Number of local authorities that are aware of the number of patients with HCV in their area18
40% Number of local authorities that had an arrangement with commissioners to co-ordinate the management of the condition19
Screening and prevention
?
£500m The cost of HCV is directly related to the severity of the disease – if treated earlier, the subsequent cost to treating HCV-related disease will be significantly reduced13 The cost to the NHS of liver disease is at least £500m, with £156m resulting from the management of HCV-liver complications, and is rising by 10% annually2 The total lifetime cost of failing to tackle HCV has been estimated to be £4.3 billion,14 with an estimated rise to £8 billion over the next 25 years2
Screening programmes in the UK target those at a higher risk of developing HCV, including past or present PWID and South Asian communities1 Screening initiatives in Scotland have demonstrated a 50% increase in the number of patients being tested and treated during the active stage of the campaign (between 2007 and 2011)15 Awareness of HCV in the UK amongst the general public still remains low and, as a consequence, diagnosis and treatment also remains low among those infected with HCV1
For more information please contact Creston Health on Gilead@crestonhealth.co.uk or +44 (0)20 8392 8040
Eating more fruits and vegetables
Infographic design and development
25% Scotland is the only UK country with a mandatory HCV Action Plan within their National Healthcare strategy
£8 billion over 25 years
This document has been produced by AstraZeneca UK who have exercised full editorial control Date of preparation August 2015 Job number 732,633.011
WORK TYPE
92% The number of PCTs in 2006 in England that were not effectively implementing a HCV Action Plan17 An audit of commissioners and local authorities in England showed that:
believe flu is serious enough to warrant vaccination17
PROJECT
In the UK there has been a 300% increase in hospital admissions and deaths from HCV-related end-stage liver disease and liver cancer in the last 12 years, from 612 in 1998 to 1,979 in 201012
Management of HCV The UK has one of the lowest treatment rates for patients with HCV in Europe2
of mums do not
32%
Direct HCV-related death rates are rising. In the UK they have more than doubled between 1996 to 2010, increasing from 98 in 1996 to 323 deaths in 20101 In England, cirrhosis and HCC-related liver transplants have been increasing steadily over the past 15 years1, but demand for liver transplants is outweighed by the demand2
20%
25%
fewer deaths a year16
References
8. 9. 10. 11. 12. 13. 14. 15. 16. 17.
The main consequences of untreated HCV are cirrhosis and hepatocellular carcinoma (HCC) and it is predicted that in England 15,840 individuals will be living with HCV-related cirrhosis or HCC by 20201
20%
* Based on U.S data
But in a recent survey
1. 2. 3. 4. 5. 6. 7.
But 25% of people are unaware that (functional) foods and drinks containing Plant Stanols are proven to lower cholesterol
2,000
10%
But in fact,
References: 1
Health Protection Agency – Hepatitis C in the UK, 2012 report. http://www.hpa.org.uk/webc/HPAwebFile/HPAweb_C/1317135237219. [Accessed December 2013]
12 Hospitals Episode Statistics (HES). The NHS Information Centre for Health and Social Care, England: Patients Episode Database for Wales (PEDW). NHS Wales Informatics Service. Health protection Scotland un association with the Information Services Division
2
The Hepatitis C Trust. The UK vs. Europe – Losing the Fight Against Hepatitis C. http://www.hepctrust.org.uk/Resources/HepC/Migrated%20Resources/Documents/Other/213_ The%20UK%20vs.%20Europe.pdf [Accessed December 2013]
14 Chief Medical Officers Report 2011, volume 1 http://www.dh.gov.uk/health/2012/11/cmo/ [Accessed December 2013]
3
WHO. 2002. Available at http://www.who.int/csr/disease/hepatitis/Hepc.pdf [Accessed December 2013]
4
Cornberg et al. A systematic review of hepatitis C virus epidemiology in Europe, Canada and Israel. Liver International. 2011: 30-60
5
Volk ML. J Antimicrob Chemother 2010; 65:1327-1329
6
CDC. Available at http://www.cdc.gov/knowmorehepatitis/Media/PDFs/FactSheet-boomers. pdf [Accessed December 2013]
7
Razavi H et al. Hepatology 2013; 57(6):2164-2170
8
Toulouse, B. Hepatitis C Fact Sheet. HCV Advocacy - NATAP.
9
NHS Choices. Hepatitis C – symptoms. Available from http://www.nhs.uk/Conditions/Hepatitis-C/Pages/Symptoms.aspx. Accessed December 2013
13 El Khoury, et al. J Med Econ. 2012;15:887-896
15 The Economist Intelligence Limited, ‘The Silent Pandemic’ report, 2012. 16 Euro Hepatitis Index 2012. Health Consumer Powerhouse. 17 The All-Party Parliamentary Hepatology Group. A Matter of Choice. 2006 18 The Hepatitis C Trust. Opportunity Knocks? An audit of hepatitis C services during the transition. [Accessed December 2013] 19 Ipsos Healthcare Combined data from the Q2/3/4 2012 HCV EU5 Therapy Monitor Base: All untreated patients with specified reason for not being on therapy, excluding patients recent diagnosis.; Patients with barriers or delaying treatment. [Data on file]
10 van der Meer AJ, et al. JAMA. 2012; 308(24):2584-2593 11 Biggins SW et al. Liver Transplantation 2012; 18:1471-1478
XXXXXXXXX December 2013
CLIENT
Infographics Median age life expectancy if starting currently available cART regimens at age 20 years
67.4
82.2
10%
YEARS
YEARS
Tolerability
20
30
40
50
25%
52%
DEPRESSION SYMPTOMATIC HIV AIDS ASYMPTOMATIC HIV MS ESRD GERD EPILEPSY US GENERAL POPULATION PROSTATE DISEASE DIABETES 10
26
YEARS
PLHIV*
Emotional well-being scores are worse for HIV patients compared to patients with other diseases, except for chronic depression
0
25.6
PLHIV
General population
LANTERN STUDY
10% of PLHIV* are expected to exhaust all currently available cART options after just 25.6 years
Only 52% of patients in a survey were satisfied with the tolerability of their medications
WEEK
STUDY
25% of PLHIV* have never spoken to their HCP about the side effects they are experiencing
Ultibro® Breezhaler® vs salmeterol/fluticasone (SFC)* in patients with stable moderate-to-severe chronic obstructive pulmonary disease (COPD), with a history of one exacerbation or none in the previous year1
40% 60
70
efficacy + safety
PLHIV
80
RESULTS
40% of PLHIV* report that their sex life has been affected completely or to a major extent by treatment side effects. Patients also express concern with side effects related to sleep disturbances, fatigue, and depression or anxiety
Up to a third of HIV-related deaths are a consequence of late diagnosis and delayed initiation of cART
63%
Only 25% of PLHIV* in the US are estimated to be virologically suppressed
*People living with HIV
SECONDARY endpoint met
Ultibro Breezhaler
27.5% of treatment switches are accounted for by adverse events in a large retrospective cohort of patients on first line treatment
63% of patients surveyed rated either minimal side effects or minimal long-term impact on the body as the most important factors when choosing ART
Features of existing ARVs can limit their use in special patient populations, such as women of child-bearing potential and those with co-infections
PRIMARY endpoint met
27.5%
Demonstrated non-inferiority vs SFC in terms of lung function (as measured by trough FEV1) at Week 262
References:
Significantly reduced the rate of moderateto-severe exacerbations by 31% compared to SFC2**
Showed superiority in improving lung function (as measured by trough FEV1; AUC0-4h) compared to SFC at Week 262
In this study, exacerbations were a pre-specified exploratory endpoint
WRAP AROUND AREA
STUDY CONDUCTED IN
744 patients
Argentina, Chile, China and Taiwan1
Chronic Obstruction Pulmonary Disease (COPD) is a chronic and highly debilitating pulmonary disease. COPD is characterised by persistent airflow limitation that makes it hard to breathe.
Ultibro Breezhaler
COPD patients suffer from day and night-time symptoms and they get worse when exercising or during an exacerbation (periods when there is a sudden increase in symptoms).
is a
There are effective treatment options available that can ease the symptoms of COPD and greatly improve a person’s quality of life. Whilst these treatments cannot reverse damage already done to the airways, early diagnosis and active management of the disease can make a real day-to-day difference.
COPD in the UK
to
hear
• COPD affects 3.7 million people in the UK, however less than 1 million are currently diagnosed.1 It is thought that this is a result of people not recognising the symptoms of COPD and instead dismissing these symptoms as result of getting older, or as just having a ‘smokers cough’ • One person dies from COPD in England and Wales every 20 minutes – equating to around 25,000 - 30,000 lives every year2
3x
Day and night-time symptoms affect COPD patients at all levels of disease severity8
Almirall is committed to improving the quality of life of people with COPD through products from its own research and development.
see
References: 1. Clinicaltrials.gov. A 26-week Treatment Randomized, Double-blind, Double Dummy Study to Assess the Efficacy and Safety of QVA149 (LANTERN). NCT01709903. Available at: http://clinicaltrials.gov/ct2/show/NCT01709903 [Accessed 17 July 2014]
4. Pavkov et al. Characteristics of a Capsule Based Dry Powder Inhaler for the Delivery of Indacaterol. CMRO 2010;26;11:2527-2533
UNDERSTANDING CHRONIC OBSTRUCTIVE PULMONARY DISEASE
COPD is recognised as the only major cause of death among women that is rapidly increasing- but awareness amongst this audience remains low6
2. Zhong N et al. Efficacy and safety of once-daily QVA149 compared with twice-daily salmeterol/fluticasone combination (SFC) in patients with COPD: the LANTERN study. [ERS abstract 700090; Session 281; Date: September 8 2014; Time].
3. EMA. 2012. Ultibro Breezhaler EU Summary of Product Characteristics. [Online] 3 October 2013. Available at: http://www.ema.europa.eu/docs/en_GB/document_li brary/EPAR_-_Product_Information/human/002679/WC500151255.pdf [Accessed 17 July 2014].
No rest from COPD symptoms
Nearly 8 in 10 patients suffer from day and night-time disturbances as a result of COPD7
and
** RR [95% CI]: 0.69 [0.48, 1.00]; p=0.048)
44%
of patients are women5
?
The prevalence rate of COPD has been increasing nearly three times faster amongst women than men6
feel
* The LANTERN study used Seretide (salmeterol/fluticasone) 50/500 mcg, which is indicated in the UK for the symptomatic treatment of patients with COPD, with a FEV1 <60% predicted normal (prebronchodilator) and a history of repeated exacerbations, who have significant symptoms despite regular bronchodilator therapy6. The patient population in the LANTERN study were stable moderate-to-severe COPD patients with a history of one exacerbation or none in the previous year2. Seretide is also known as Advair® and Accuhaler is also known as Diskus®. Seretide, Advair, Diskus and Accuhaler are registered trademarks of the GlaxoSmithKline group of companies.
• Emergency admissions for COPD are the second highest of any disease area in the UK, resulting in excess of 1 million bed days3
of those with COPD are less than 65 years old and
,
that they have taken the full dose correctly 4,5
• COPD is one of the most costly inpatient conditions treated by the NHS, with hospital admission costs related to COPD estimated at over £310 million per annum4
50%
once-daily
maintenance bronchodilator treatment approved in the EU to relieve symptoms in adult patients with COPD3
The Breezhaler® inhalation device allows patients
There is continued low public awareness of COPD. There is therefore a need to raise the profile of the disease among people in order to support accurate recognition of symptoms and to educate on effective ways COPD can be treated.
COPD has historically been seen as a disease that affects old men; recent estimates suggest that
56 sites
ACROSS
UNDERSTANDING CHRONIC OBSTRUCTIVE PULMONARY DISEASE
The changing face of COPD
at
5. Onbrez® Breezhaler® (indacaterol) EU Summary of Product Characteristics. [Online] Available at: http://www.ema.europa.eu/docs/en_GB/document_li brary/EPAR_-_Product_Information/human/001114/WC500053732.pdf [Accessed 17 July 2014] 6. Seretide® Summary of Product Characteristics [Online] Available at: https://www.medi cines.org.uk/emc/medicine/2317/SPC/Seretide+100,+250,+500+Accuhaler [Accessed 17 July 2014]
Chronic Obstructive Pulmonary Disease (COPD) is a progressive and highly debilitating disease that affects the lungs. COPD is characterised by persistent airflow limitation, typically due to inflammation of the bronchi (airways) and damage to the alveoli (air sacs). Symptoms include: breathlessness, cough, tight chest, wheezing, and producing excess mucus.
Night-time symptoms are an under recognised unmet need of COPD. Patients with both day-time and night-time symptoms are more likely to have severe breathlessness, more exacerbations and receive a higher number of maintenance products than those with day-time symptoms only8
COPD patients suffer from day-and night-time symptoms, which become worse when exercising or during an exacerbation (a ’flare-up’ of symptoms). COPD affects many aspects of a patient’s daily life.
1. British Lung Foundation. Invisible Lives - Chronic Obstructive Pulmonary Disease (COPD) - finding the missing millions Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed August 2014 2. HSE. Chronic Obstructive Pulmonary Disease. Available at http://www.hse.gov.uk/statistics/causdis/copd/copd.pdf. Accessed August 2014 3. British Lung Foundation. Ready for home? - Improving hospital discharge care for people living with COPD. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed August 2014 4. National Institute for Health and Care Excellence. NICE Costing Report. Chronic Obstructive Pulmonary Disease. NICE CG 101. 2011 5. Rennard, S et al. Impact of COPD in North America and Europe in 2000: subjects’ perspective of Confronting COPD International Survey. Eur Respir J. 2002. 20:799-805 6. British Lung Foundation. Femme-Fatality – The rise and rise of COPD in women. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed August 2014 7. Price D, Small M, Milligan G. Prevalence and impact of night-time symptoms in COPD patients-results of a cross-sectional study in five European countries. Presented at: 4th World Asthma & COPD Forum; 2011; Paris, France 8. Price D, Small M, Sayers J. Characteristics of COPD patients experiencing night-time symptoms-results of a cross-sectional study in five European countries. Presented at: 4th World Asthma & COPD Forum; 2011; Paris, France
Date of preparation: September 2014 Job code: UKACL2344a
There are effective treatment options available that can ease the symptoms of COPD and improve a person’s quality of life. Whilst these treatments cannot reverse damage already done to the lungs, early diagnosis and active management of the disease can make a real day-to-day difference. There is continued low public awareness and correct diagnosis of COPD. There is therefore a need to raise the profile of the disease among people in order to support accurate recognition of symptoms and to educate on effective ways COPD can be treated.
COPD in the UK • COPD is common. It affects approximately 3.7 million people in the UK, however less than 1 million are currently diagnosed1 • One person dies from COPD in England and Wales every 20 minutes – equating to around 25,000 deaths every year2 • Emergency hospital admissions for COPD are the second highest of any disease area in the UK, resulting in excess of 1 million ‘bed days’ in hospitals each year3 • COPD is one of the most costly in-patient conditions treated by the NHS, with hospital admission costs related to COPD estimated at over £310 million per annum4
DIABETES, A GLOBAL PANDEMIC.
A health problem that has unified the science community globally in order to find a solution. The International Diabetes Foundation predicts that by 2035 one in ten of the world’s population will be living with diabetes, the implications of which permeate every corner of society. Given the number of people currently being treated for Type 1 or Type 2 diabetes worldwide, it is often assumed that healthcare professionals are well-versed in the range of treatment options available, identifying which treatment is suitable for which patient, and understanding when to initiate and intensify insulin regimens.
case. The overwhelming theme from the feedback was that messaging around the positioning of diabetes treatments needs to be less complex. How does human insulin differ from analogues? What exactly are the clinical benefits of analogues and do these benefits justify the increased cost? Clear, simple messaging will ensure that GPs have confidence in prescribing the right treatment and can defend and rationalise their decision when challenged against a range of cost and guideline restrictions.
This situation analysis has been developed to collate the key interviews and media desk top research (including social media) undertaken by Red Door Communications (RDC) for However, having spoken with a broad the development of our strategic range of healthcare professionals across recommendations and considerations different markets and disciplines within for the Novo Nordisk Modern diabetes care as part of our research, Insulin brands and devices portfolio it appears that this is not always the communications activities.
PROJECT
WORK TYPE
Infographic design and development
Print and digital media
N MODELRIN INSOUUND AR ORLD: THE W
The changing face of COPD Diabetes Experts spoken to
KATRIN HERTRAMPF
PROFESSOR DR HELLMUT MEHNERT
Diabetes Nurse
Munich-Schwabing Hosptial
Germany
Germany
DEBBIE HICKS Senior Diabetes Specialist Nurse Hull Royal Infirmary, UK
DR MATTHEW CAPEHORN
PROFESSOR TONY BARNETT
Clinical Manager
Emeritus Chair of Medicine
Rotherham Institute of Obesity, UK
Birmingham Heartlands Hospital, UK
GWEN HALL Diabetes Specialist Nurse Solent NHS Trust, UK
• COPD has historically been seen as a disease that affects old men; however, recent estimates suggest that the mean age of those with COPD is less than 65 years old and around 44% of patients are women5 • The incidence rate of COPD has been increasing nearly three times faster amongst women than men6
No rest from COPD symptoms
TS
SIGH PERT IN
DR ROGER HENDERSON
PROFESSOR MELANIE DAVIES
GP and Media Medic
Professor of Diabetes Medicine
Telford, UK
Leicester General Hospital, UK
DR MICHAEL FEHER
PAUL RYAN
DR MARCIA NERY
Consultant in Diabetes & Clinical Pharmacology
Deputy Head of Contracts
Supervising docator of the Endocrinology and Metabolism Hospital das Clinicas medical school of the University of São Paulo, Brazil
Hertfordshire, UK
Chelsea and Westminster, UK
• Nearly 8 in 10 patients suffer from day-and night-time disturbances as a result of COPD7 • Individual patients rank the importance of various COPD symptoms differently; however, in general, shortness of breath is the symptom that causes them the most concern8 • COPD patients at all levels of disease severity can be bothered by night-time symptoms9 • Night-time symptoms are an under-recognised unmet need of COPD. Patients with both day-time and night-time symptoms are more likely to have severe breathlessness, more exacerbations and receive a higher number of maintenance treatments than those with day-time symptoms only9
DR KAMINI D LAKHIANI Endo-Diabetologist Sadhana Proactive Clinic, India
EX
GENERAL INSIGHTS:
DIABETES TREATMENT REGIME COST-EFFECTIVENESS:
HUMAN VS. ANALOGUE INSULIN
TYPE 1 DIABETES
TYPE 2 DIABETES
• There is a ‘honeymoon period’ straight after diagnosis, when an aggressive treatment regime is not always necessary
• Treatment regime is more variable for these patients and it is difficult to assess when to start insulin
• A basal bolus system is required, using a mix of rapid and intermediate treatment:
• Human insulin is prescribed more in countries where cost is an issue
– x2 injections taken daily taken at the start of treatment
• Countries such as India, China, Australia, Western Europe and Canada are richer, so analogues tend to be prescribed more. In addition:
– This will then increase to more aggressive treatment – x3 injections of rapid-acting insulin before each meal and a 4th injection of a longer- acting insulin taken before bedtime to provide background insulin • There is no pressure for HCPs to use older NPH insulin (which is cheaper) in T1D because hypos are a bigger problem (and this has a strong evidence base) – meaning the cost argument is a lot easier
– GLP1/basal treatment in combination tends to be prescribed more – T1D tends to be treated more aggressively in these countries
• In Germany, initiation on insulin happens much earlier than in France or the UK; it can take up to 10 years in the UK and even longer in France • NovoRapid is common in patients with T1D. In T2D its use is pushed back by GLP1 and basal combo – but the rapid component is often still required (some patients don’t respond well to long-acting and the disease is progressive) • Diabetes treatment regime in Canada, Australia and Turkey is similar to the UK • Most countries adhere to the ADA, EASD and IDF guidelines – Canada has its own guidelines (Canadian Diabetes Association)
Brazil: For type 2 diabetes, meta-analysis shows that the use of analogues is not cost- effective; in my opinion, it is only patients with type 2 diabetes under intensive insulin therapy and with high risk of hypoglycaemia who are recommended the analogous. Dr Marcia Nery
UK: There is more pressure to use NPH insulin (intermediate-acting) – it is known that older insulins increase hypos, but the recommendation from NICE is that patients should be switched only when hypos occur. Professor Tony Barnett
Germany: Unfortunately the German health system does not treat life quality as a “hard” factor. The factor that makes the most impact on the reimbursement of treatment costs is the Hba1c level. Katrin Hertrampf
Germany: Still the 'human' insulins are not worse than the insulin analogues, they are just more rigid and don’t allow as much flexibility. Especially for kids and young adults the insulin analogues are an advantage. Katrin Hertrampf
UK: The argument for MI versus HI is not that solid: HI is seen as moderately effective and cheaper. Paul Ryan
UK: When considering modern insulins, I would use the NICE guidance and have a look at what is best value for money, at what is the most cost effective for the patients and the NHS. Debbie Hicks
India: I very rarely prescribe human insulin; only for patients who cannot afford analogues as they are too costly. Kahmini D Lakhiani
Germany: In the beginning, and during the course of the insulin effect, analogues do have a major advantage over human insulin. Prof. Dr. Hellmut Mehnert
1. British Lung Foundation. Invisible Lives – COPD – finding the missing millions. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed November 2015 2. Health and Safety Executive. Chronic Obstructive Pulmonary Disease. Available at http://www.hse.gov.uk/statistics/causdis/copd/copd.pdf. Accessed November 2015 3. British Lung Foundation. Ready for home? – Improving hospital discharge care for people living with COPD. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed November 2015 4. National Institute for Health and Care Excellence. NICE Costing Report. COPD. NICE CG 101. 2011 5. Rennard, S. et al. Impact of COPD in North America and Europe in 2000: subjects’ perspective of Confronting COPD International Survey. Eur Respir J 2002;20:799–805 6. British Lung Foundation. Femme-Fatality – The rise and rise of COPD in women. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed November 2015 7. Price D, et al. Prevalence and impact of night-time symptoms in COPD patients – results of a cross-sectional study in five European countries. Presented at: 4th World Asthma & COPD Forum; 2011; Paris, France 8. NICE Clinical Guidelines, No. 101. COPD. Available at: http://www.ncbi.nlm.nih.gov/books/NBK65029/ Accessed November 2015 9. Price D, et al. Characteristics of COPD patients experiencing night-time symptoms-results of a cross-sectional study in five European countries. Presented at: 4th World Asthma & COPD Forum; 2011; Paris, France
Date of preparation: November 2015 Job code: 930,527.011
CLIENT
Infographics
3.7 M LL ON people are estimated to be living with COPD in the UK, yet only 900,000 people have been diagnosed with the disease
IMPACT OF CVD IN THE UK 175,000
7 million
people estimated to be living with cardiovascular disease (CVD) in the UK British Heart Foundation. Cardiovascular Disease Statistics Factsheet. Available at https://www.bhf.org.uk/research/heart-statistics [last accessed March 2015].
minutes
British Heart Foundation. Cardiovascular Disease Statistics Factsheet. Available at https://www.bhf.org.uk/research/ heart-statistics [last accessed March 2015].
£19bn
British Lung Foundation. Invisible Lives – COPD – finding the missing millions. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed April 2015
The estimated total cost of premature death, lost productivity, hospital treatment and prescriptions relating to CVD each year in the UK
768,216.011 | May 2015
It is estimated that
3
heart attacks (MI) in the UK each year; that's one every three minutes
British Heart Foundation. Cardiovascular Disease Statistics Factsheet. Available at https://www.bhf.org.uk/research/heart-statistics [last accessed March 2015].
160,000
deaths caused by CVD in the UK each year
British Heart Foundation. Cardiovascular Disease Statistics Factsheet. Available at https://www.bhf.org.uk/research/heart-statistics [last accessed March 2015].
2.8 million
people in the UK are living with undiagnosed COPD
CVD is projected by World Health Organization (WHO) to remain a substantial contributor to global deaths, causing an estimated 22.2 million deaths in 2030
110,000 men and 65,000 women in the UK suffer a heart attack each year
World Health Organization. Global Status Report on Noncommunicable Diseases: 2014. Available at http://www.who.int/nmh/publications/ncd-status-report-2014/en/ [last accessed February 2015].
1/ 5
British Heart Foundation. Cardiovascular Disease Statistics Factsheet. Available at https://www.bhf.org.uk/research/heart-statistics [last accessed March 2015].
~1 in 5 patients who were event free for the first year post-MI suffered an MI, stroke or death within 3 years [APOLLO 4-country analysis]
Only half of patients with coronary heart disease use 3 or more of the recommended treatments 5 years after their cardiovascular event World Heart Federation. Secondary cardiovascular disease prevention and control. July 2014. http://tinyurl.com/pzvo2vn [Last accessed March 2015].
Rapsomaniki E, et al. ESC Late. Breaking Registry presentation 2014.
2
This document has been produced by AstraZeneca UK Date of preparation March 2015 | 705,713.011
minutes
One person dies from COPD in England and Wales every 20 minutes resulting in around 25,000 deaths every year Health and Safety Executive. Chronic Obstructive Pulmonary Disease. Available at: http://www.hse.gov.uk/statistics/causdis/copd/copd.pdf. Accessed April 2015
Tecfidera is a new oral treatment for adult patients with relapsing remitting multiple sclerosis (MS)1 – the most common type of MS2
Tecfidera is licenced for patients with relapsing remitting MS1
THE BENEFITS OF TECFIDERA
x2
Tecfidera is taken twice daily with food1
Causes of prostate cancer The factors that determine the risk of developing prostate cancer are not well known, although a few have been identified. The well-established risk factors for prostate cancer are:4
Increasing age
Ethnic origin Genetic predisposition Unhealthy diet Smoking
about 80% of men who reach the age of 80 have prostate cancer cells in their prostate
Anxiety and depression, stress or loss of control, and problems in coping
Treatment options for prostate cancer Treatment options are based on the stage and grade of the disease. When the prostate cancer is more advanced, and has spread to other parts of the body, treatment includes reducing the level of testosterone (a male hormone). Prostate cancer cells need testosterone, an androgen, to grow. The cellular effects of androgens are mediated via the androgen receptor.7
Hormonal treatment is used to lower the level of a man’s testosterone (also known as androgen-deprivation). This in turn can shrink the cancer, reduce prostate-specific antigen (PSA) levels and control symptoms.8
The list price for Tecfidera will be £17,900 per annum
HOW TECFIDERA WORKS The mechanism of Tecfidera is not fully understood. It is believed to reduce inflammation via the Nrf2-dependent antioxidant pathway1
90%
Reduce the rate of MS relapses by 53% (0.17 vs. 0.36, p<0.001)3 and 44% (0.22 vs. 0.40, p<0.001)4 vs. placebo at 2 years
38%
Reduce the number of gadoliniumenhancing lesions on MRI by 90% (0.1±0.6 vs. 1.8±4.2, p<0.001)3 and 74% (0.5±1.7 vs. 2.0±5.6, p<0.001)4 vs. placebo at 2 years
SIDE EFFECTS
27%
Delay disability progression by up to 38% 38% (16% vs. 27%, p=0.005)3 and 21% (13% vs. 17%, p=ns)4 vs. placebo at 2 years
27% of patients on Tecfidera had an MS relapse in 2 years, vs. 46% of patients treated with placebo (p<0.001)3
The most common side effects of Tecfidera are flushing and gastrointestinal problems (e.g. diarrhoea, nausea and abdominal pain)1
1 million
These side effects tend to begin early in the course of treatment and may continue to occur intermittently throughout treatment1
TF-GBR-0068 January 2014
Burden of Chronic Spontaneous Urticaria (CSU)
CSU is a serious, chronic and distressing skin condition that is difficult to diagnose and manage.
SYMPTOMS
1-4
‘bed days’ in hospitals each year
768,216.011 | May 2015
6
most common cause of cancer death in Europe
In two pivotal phase lll studies, Tecfidera has been shown to:
53%
British Lung Foundation. Ready for home? – Improving hospital discharge care for people living with COPD. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed April 2015
90,000 deaths every year3
every minutes
TECFIDERA (DIMETHYL FUMARATE)
768,216.011 | May 2015
Emergency hospital admissions for COPD are the second highest of any disease area in the UK, resulting in excess of
resulting in more than
one man
Men with advanced prostate cancer often report feelings of:5,6
British Lung Foundation. Invisible Lives – COPD – finding the missing millions. Available at: http://www.blf.org.uk/Page/Special-Reports. Accessed April 2015 768,216.011 | May 2015
3
is the
with a mortality rate of at least
rd
Prostate cancer
! !! ! !! ! ! !
!
How can Red Door Communications’ Consumer Health experience benefit
GSK’s Consumer Healthcare Product Portfolio? Red Door’s consumer health team comprises outstanding consultants who have worked at some of the UK’s leading agencies supporting some of the UK’s best known consumer brands with innovative, impactful and award winning campaigns
Extensive experience of running busy press offices including the generation of newshooks and media content, the creation and development of social media communities and online engagement, media events and briefings
!!
COMPLICATIONS
2
There is no specific external trigger for CSU, but the autoimmune system may play a role.
zzz
CHRONIC (LASTING FOR AT LEAST SIX WEEKS)
SPONTANEOUSLY OCCUR
SLEEP DEPRIVATION
DEPRESSION RED HIVES (WHEALS)
DEEP TISSUE SWELLING (ANGIOEDEMA)
ITCH
PREVALENCE
1-2
61% ONLY WHEALS
33% WHEALS AND SWELLING 6% ONLY SWELLING
TREATMENT
Antihistamines are the current mainstay of treatment, but more than 50% of people with CSU on approved antihistamine doses do not achieve symptom relief.
DURATION
2
People with CSU who experience deep tissue swelling (angioedema) may have a greater chance of CSU lasting for >12 months or longer.
Symptoms remain uncontrolled even in many people with CSU receiving
4x
The disease generally lasts 1–5 years but can last for decades.
Price D, et al. Prevalence and impact of night-time symptoms in COPD patients – results of a cross-sectional study in five European countries. Presented at: 4th World Asthma & COPD Forum; 2011; Paris, France 768,216.011 | May 2015
A proven track record of delivering measureable and meaningful results for brands in the area of dermatology, weight loss, oral healthcare, colds and flu, VMS and naturals, analgesics and pain relief, gastro-enterology, smoking cessation, eye care, nutrition and allergy
Evidence of successful consumer and stakeholder recruitment for health related campaigns and services
1. Primary Care Dermatology Society website. Available at http://www.pcds.org.uk/clinical-guidance/urticaria-spontaneous-syn.-chronic-ordinary-urticaria *[Last accessed August 2013] 2. Maurer M et al. Allergy. 2011;66:317–330. 3. Zuberbier T et al. Allergy. 2009;64:1417–1426. 4. Maurer M et al. Br J Dermatol. 2013 Feb;168(2):455-456. 5. Zuberbier T et al. Clinical and Experimental Dermatology. 2010;35:869-873.
PSORIASIS
up to four times the approved antihistamine dose.
Approximately 1/5 of people with psoriasis have moderate to severe psoriasis
however, recent estimates suggest that the mean age of those with COPD is less than 65 years old and around 44% of patients are women
LESS THAN
65 YEARS OLD
44% WOMEN
Rennard, S. et al. Impact of COPD in North America and Europe in 2000: subjects’ perspective of Confronting COPD International Survey. Eur Respir J 2002;20:799–805 768,216.011 | May 2015
A thorough, inside track on what makes news and media coverage in broadcast, digital, social, national, regional, specialist and trade titles
A full suite of design, digital, video production and medical education skills on site
Creative brains and skilled practitioners which enable Red Door to marry Brilliant Basics with Intelligent Innovation on behalf of our clients
Please contact Julia Harries on +44 (0) 20 8392 8044 or email: jharries@rdcomms.com
PROJECT
WORK TYPE
Infographic design and development
Print and digital media
MOST COMMON SYMPTOMS 18
ITCHING PAIN
PEOPLE IN THE UK MAY HAVE PSORIASIS5
A wealth of examples of effective collaborations and joint work including celebrity and ambassador recruitment
1-4
PSORIASIS CAN BE MILD, MODERATE OR SEVERE6
AN ESTIMATED
Red Door is the most rated agency by UK health journalists and an Executive Committee Member of the Medical Journalists’ Association
XOL13-C082 September 2013
A COMMON, CHRONIC AND INFLAMMATORY AUTOIMMUNE DISEASE
1.8 M LL ON COPD has historically been seen as a disease that affects old men;
EMOTIONAL UPSET
2
At any given time, 0.5-1% of the global population is affected by CSU. Women are more likely than men to be diagnosed.
5
ANXIETY
SOCIAL ISOLATION
*Typical symptom presentation
Nearly 8 in 10 patients suffer from night-time disturbances as a result of COPD5
LACK OF ENERGY
MILD Less that 3% of the body has psoriasis
MODERATE
SEVERE
3%-10% of the body has psoriasis
More than 10% of the body has psoriasis
1% = Surface area of the hand
THICK, RED SKIN SCALING
EFFECTS ON QUALITY OF LIFE
6-10
The effect of psoriasis on patients’ quality of life is similar to diseases such as cancer, heart attack, arthritis, type 2 diabetes and depression. People with more severe forms of psoriasis have a significantly reduced life span.
75%
FEEL UNATTRACTIVE7
77%
54%
FEEL DEPRESSED7
31%
HAVE FINANCIAL DISTRESS7
SAY IT LEADS TO SEXUAL DIFFICULTIES10
PSORIATIC ARTHRITIS17
There is no cure for psoriasis and up to 78%7 of patients express low to moderate satisfaction with their treatment. This indicates the remaining unmet need for therapies that act faster and longer to relieve the symptoms of psoriasis.
1. The National Psoriasis Foundation website. Accessed 13 June 2013
SAY IT AFFECTS WHAT THEY WEAR10
27%
PATIENTS WITH PSORIASIS SAY THAT IT IS A PROBLEM OR A SIGNIFICANT PROBLEM, IN THEIR EVERYDAY LIVES10
TREATMENT FAILURE10-13,16
56%
7. Krueger G, Arch Dermatol 2001;137:280-284
30%
of patients are affected
8. Rapp SR et al. JAAD1999;41 (3 Pt 1):401-7
16. Sterry W et al. Br J Dermatol. 2004 Aug;151 Suppl 69:3-17
9. Guenther L et al. J Cutan Med Surg. 2009
17. Bowcock AM, Hum. Mol. Genet. 2004;13 (suppl 1): R43-R55 18. Lebwohl M et al. Int J of Dermatol. 2013 Apr; doi: 10.1111/j.1365-4632.2012.05798.x.
4. Herrier R, Am J Health-Syst Pharm 2011; 68:795-806
10. Dubertret L et al. Br J Dermatol 2006;155:729-736
5. The Psoriasis Association. ‘What is Psoraisis?’ 2013
11. Stern R S et al. J Investig Dermatol Symp. 2004
6. National Psoriasis Foundation, Psoriasis Severity. Available at http://www.psoriasis.org/about-psoriasis/treatments/severity [Accessed August 2013]
12. Christophers E et al. J Eur Acad Dermatol Venereol. 2006;20:921-925
19. Abuabara K et al. Br J Dermatol. 2010 Sep;163(3):586-92
13. Mason AR et al. Cochrane Database Syst Rev. 2009;15;(2):CD005028
20. Gelfand JM et al. Arch Dermatol. 2007 Dec;143(12):1493-9
17,19,20
PSORIATIC ARTHRITIS DEPRESSION DIABETES HEART DISEASE
15. Ljosaa TM et al. J Eur Acad Dermatol Venereol. 2012;26:29–35
2. Nestle FO et al. N Engl J Med 2009; 361(5):496-509 3. Brezinski EA et al. PLoS ONE; 7(4):e33486
14. Langley R G B et al. Ann Rheum Dis. 2005; 64(Suppl II):ii18–ii23
CO-MORBIDITIES
PSO13-C033 October 2013
CLIENT
Infographics YOUR
ADVANCED PROSTATE CANCER
How do the chances of surviving a heart attack differ across London?
HEART
MEET BOB Bob is a London cabbie whose been told by his doctor that he is at risk of a heart attack. What Bob doesn’t know is that depending on where he lives – or works - in London, he is more likely to survive from a heart attack. See how his risk varies in a typical day.
2
16
1
CHISWICK
HIGH ROAD
DRAFT IN THE CAPITAL? LONDON BOROUGHS
7
Percentage of hospital patients who die in the 30 days following a heart attack
2
BOB’S HOME
RUISLIP
Bob’s starts out from his home in Ruislip where his chances of survival are relatively poor in comparison with other boroughs - 20.6% of patients who go into hospital following a heart attack (STEMI) die within 30 days.
6
10
12
3
Deaths above national average
No % available - less than 5 deaths in 2011/2012
1
1
Hillingdon
17 Southwark
2
Harrow
18 Newham
3
Watham Forest
19 Bexley
4
Merton
20 Ealing
5
Hackney
21 Barking and Dagenham
6
Barnet
22 Camden
7
Westminister
23 Greenwich
8
Havering
24 Hammersmith and Fulham
9
Tower Hamlets
25 Hounslow
27 Kingston upon Thames 28 Lambeth
29 Lewisham
30 Richmond 31 Sutton
16 Enfield
32 Wandsworth
OFF TIME IN
7
25
26 Kensington and Chelsea
15 Croydon
4
24
32
30
7
ALGATE STATION BACK
TO UXBRIDGE
On his way home, Bob sees some angry commuters outside Aldgate station – the Metropolitan line is down. Bob takes them home, which is at the other end of the line, in Uxbridge. On the journey, the death rate following 30 days after hospital admission for heart attack doubles from 10.3% to 20.6%.
6
4
27
9
21
18
17
28
23
29
LEWISHAM
Bob picks up an MP leaving the House of Commons to go home to Lewisham for the evening, if Bob has a heart attack here his chances of survival dramatically improve as fewer than 5 people die within 30 days of hospital admission following a heart attack.
31
15
8
What is prostate cancer?
CAMDEN
MARKET
Bob then picks up a group of friends who want to visit Camden market. Once in Camden, Bob’s chances of survival improve again – with less than 5 people dying within 30 days of hospital admission following a heart attack in Camden.
4
6
26
11 Haringey
14 Islington
20
2
10 Bromley
13 Redbridge
5
22
1
3
13
5
14
Deaths on or below national average
12 Brent
3
Bob spots a golfer leaving Rusilip golf course who is meeting his son for lunch on Chiswick High Road. If Bob has a heart attack in this borough, his chances of survival improve significantly – just 6.1% of those admitted to hospital following a heart attack die within 30 days.
19
The prostate gland is part of the male reproductive system. About the size of a walnut, its role is to secrete fluid that nourishes and protects sperm.
SLOANE
STREET
Bob drives south and picks up a couple on Oxford Street shopping for engagement rings. He takes them to Sloane Street where they can have their pick of jewellery shops. On Sloane Street, Bob’s chances of survival are again good – with less than 5 people dying within 30 days of admission following a heart attack in the Borough of Kensington and Chelsea.
In some men, prostate cancer cells may also spread beyond the prostate and move to other parts of the body, most commonly the
bones or lymph nodes
(small, bean-shaped glands throughout the body).
This is referred to as advanced or metastatic prostate cancer.
10
5
Prostate cancer refers to the growth of cancerous cells within this gland. Prostate cancer occurs when abnormal cells, supported by male hormones such as testosterone, begin to grow uncontrollably to form tumours.
CITY OF
WESTMINISTER
Prevalence
Bob sees a lawyer in Sloane Square needing a lift to the City for a business meeting. In the City of Westminster, Bob’s chances of survival start to drop, with 10.9% of hospital admissions following a heart attack resulting in death within 30 days.
Prostate cancer has emerged as the most common non-skin cancer in men in Europe, accounting for over of all cancer diagnoses in men1
20%
About
10-20%
of patients present with advanced stage disease2
PARKINSON’S
PREVALENCE OF PARKINSON’S
Parkinson’s is caused by a lack of a chemical called
DOPAMINE in affected people’s brains Around
127,000
Parkinson's is often
people in the UK have Parkinson’s1
HOUR someone in the UK is told
associated with
Every
older people
and most people who are diagnosed with Parkinson’s are over the age of 501
they have Parkinson's1
SYMPTOMS
1 in 20 people newly diagnosed is under the age 1 of
40
Did you know... Michael J Fox was diagnosed with Parkinson’s when he was just 29 years old (MJFox foundation)2
TREATMENT Symptoms are different for everyone,
Some treatments for Parkinson’s are
chemical BUILDING BLOCKS that the
but common symptoms include tremor, stiffness, problems with movement
and walking, pain, depression, fatigue3 and gastrointestinal problems4
body can convert into dopamine1
Other treatments called dopamine agonists act like dopamine to stimulate the nerve cells. Some dopamine agonists can be used to treat or reduce off time1
WHAT IS OFF TIME?
OFF TIME is when treatment that
helps the brain to produce more dopamine starts to ‘wear off’ before the next dose5
OFF PERIODS CAN BE
When the treatment
‘WEARS OFF’ the symptoms of Parkinson’s RETURN5
6,13
Patients can experience ‘dose failures’ where they receive no clinical benefit from treatment. This is thought to be due to problems with the medicine being absorbed in the gastrointestinal tract and also with the medicine entering the brain from the bloodstream once absorbed8 Date of Preparation: February 2014 APO1-0214-0429
6
A part of Health Unlimited
A six year old, specialist healthcare communications company, with a clear position in the market place as a boutique agency,
YEARS offering a personal and responsive service to our clients, which also happens to be Communiqué Small Consultancy of the Year!
Here is a quick overview of the key things you might like to know about us. Our success comes down to three critical ingredients our ethos, our clients and our team members 1 Our ethos can be defined by our core values: • Relationship focused • Positive challenge • Refreshing • Nimble
2
We have really great client relationships; everybody will tell you that – but there are ways of measuring it! • Scores from an independent client satisfaction survey, repeated every year (RAM Feb 2014) � 8.9 for ‘chemistry and working relationship’ � 8.4 for ‘how likely would you be to recommend the agency to a friend or colleague’ � 8.2 for ‘quality of people, resource and skills’ • The average RAM score based on 30,000 client interviews is 7.0 (1 lowest, 10 highest) We have two long standing client relationships of 5 years (and counting) The average length of client relationship is 3.2 years
staff turnover for the last three years 3 0% resulting in consistency for clients, effective teamwork and excellent team morale
AWARDS 2 wins (PMEA Award for Launch Excellence and did we mention we won Communiqué Small Consultancy of the Year?)
2014
in numbers
Access to over
Average client satisfaction rating of
8.2 8.2 (RAM)
decade (IMS data)
1/3
Secured a guinness world record for Hep C with
26,204
across 16 countries within Chemia, our Health Unlimited global network
participants
is a great place to work (Your Voice)
The launch of the
first cannabis –based treatment
A NICE HTA methodology change
PROJECT
WORK TYPE
Infographic design and development
Print and digital media
Most successful NGO video on YouTube
Helped three of our clients to trend globally on twitter! With over
90,000 Tweets alone for #worldcancerday
£18m
Drove
1,146,255
Youtube video views for one client campaign Drove
49%
Industry awards for one consumer health campaign Secured
#
of uk population by driving them into pharmacy when suffering cold and flu rather than wasting valuable GP time
WON 5
100% of staff thinks Liberation Unlimited
OUR TEAM HAS BEEN RESPONSIBLE FOR:
The most successful pharmaceutical launch in the last
Changed behaviour of
3 days
20 agency members
140 healthcare marcomms consultants in London to support
programmes via Health Unlimited
3 finalist rankings
Helped Boots sell out of OTC product following expertiential campaign in
Worth of funding secured ahead of health technology appraisal decision
Sales increase of health testing device during 3 month campaign period
CLIENT
Invites & Events
HERE ARE OUR 10 REASONS WHY EVERY COMPANY SHOULD EMBARK ON THE 1010 CHALLENGE:
1
IT’S A LOT HARDER THAN IT LOOKS
As a PR consultancy we pride ourselves on our strategic thinking and commercial acumen. When we were set the challenge, the fighting talk was rife with lots of big and bold ideas. However, when it came to the crunch, making money from £10 is much harder than it seems, which was all part of the fun of the challenge. In this time of shrinking budgets what better way to encourage people to be doing more with less.
2
3
IT’S GOOD TO CREATE SOME HEALTHY COMPETITION
MORALE HAS NEVER BEEN HIGHER
You can run the challenge as individuals but we decided to organise people into teams so they had the chance to pool their cash for greater spending power! A word of warning though, an ultracompetitive bunch can mean the competition gets fierce!
For the month when we ran the challenge the office was abuzz with bake offs, socials and general merriment. If your company has undergone recent change, you have new joiners or you’ve just finished a particularly busy period it could be a great time to do the 1010 and give everyone a real morale boost.
4
5
A MONTH MAY NOT BE ENOUGH
THERE ARE SOME SECRET ENTREPRENEURS AMONGST US
Entrepreneurship often doesn’t shine through unless you’re given the right opportunity. The 1010 challenge unlocked some really ingenious ideas, and marked out the Richard Branson’s amongst us.
We ran the challenge over a month, but in hindsight, a little longer may have been optimal to make sure all teams had a chance to run their events, sell their wares and take on their challenges to avoid charity fatigue setting in.
Health Unlimited: Clear Desk Policy Please ensure you follow the guidelines:
6
THE 1010 CHALLENGE IS INFECTIOUS
Everyone we told about the challenge loved the concept and wanted to get on board. One team decided to run a social media auction and asked local businesses to give prizes. The generosity was unbelievable and prizes were donated by restaurants, gyms, spas, the list goes on. Of course this was partly down to our charm ;-), but part of the success was also down to people really buying into the intriguing concept of multiplying a humble tenner. Everyone was keen to help out.
7
IT SHOWCASED ALL OUR SKILLS
Who knew we had a qualified beautician, singer, artist, cook, mountain climber and long distance cyclist in our midst? The challenge was a great way to get to know each other and showcase all our skills.
8
IT IS A FORM OF TRAINING
We often sit in boardrooms for long theory based sessions and spend a lot of cash on training budgets in the process. Our Senior Management were surprised at what great hands on training the challenge was, and how many company objectives it covered off: encouraging creativity, team work, entrepreneurship, leadership and CSR. The challenge makes business sense as well as being a great thing to do for charity.
9
IT HAS A REAL MESSAGE AND LINK TO THE END CAUSE
Did you know that the seed capital HOPEHIV provides the young people it serves to start up their own business is often just £10? It seems much more meaningful to support a fundraising activity that has such a strong link with the cause you’re working towards. To be able to see potential in a modest amount is exactly the message of the 1010. We multiplied our tenner by ten to give the opportunity for someone to start a business that could be life sustaining.
BUT MOST OF ALL £4000
10
IT HAS A SUSTAINABLE IMPACT ON THE LIVES OF OTHERS
We managed to raise £4,000 through our challenge. When we’d finished, HOPEHIV were able to let us know how that cash could be potentially spent and the lives it will impact. We found out that if 30 people took part, each would have raised enough to have transformed 7 lives through a great project called AFREDA. The project based in Tanzania works with elderly grannies and female guardians who provide for AIDS orphans to offer training in entrepreneurship, credit management and group leadership. There are few fundraising challenges through which you can measure the direct impact, which is truly hopeful.
30
£10
IF PEOPLE TOOK PART, EACH WOULD HAVE RAISED ENOUGH TO HAVE TRANSFORMED LIVES
x7
7
PROJECT
WORK TYPE
Invites & events design and development
Print and digital media
1
2
3
4
5
FIRST THING:
WHEN AWAY FROM YOUR DESK:
THROUGHOUT THE DAY:
AFTER MEETINGS:
END OF DAY:
Place documents needed for immediate work on your desk only. Other documents can be locked away.
All sensitive information must be removed from the desk surface and filed or locked up.
Place sensitive documents in t he confidential waste in the bins provided.
Ensure that any information is removed from white boards, walls, desks etc.
Lock laptops in your pedestal or take it home with you.
PLAN AND ORGANISE YOUR DAY:
LOCK YOUR COMPUTER.
CONFIDENTIAL WASTE.
REMOVE INFORMATION
THERE WILL BE CONSEQUENCES FOR POLICY NON-COMPLIANCE!
ALWAYS LEAVE A CLEAN, CLEAR DESK.
CLIENT
Invites & Events DAYAW L PAYPU B CR 28th AU GUST 20 1 4
5
THE
TION DONA In aid of Creston’s
GOLDEN TICKET
LOCATION: CENTRAL NEAREST STATION WATERLOO/ BLACKFRIARS/ SOUTHWARK
Charity Partner
AS CHOSEN BY
JOIN US FOR A FUN FILLED EVENING AT YOUR FAVOURITE LOCALS
If you have any questions or would like to buy tickets, please contact Emily Blakemore @ eblakemore@rdcomms.com
At each of the stops you’ll also be in with the chance to win a special pub-related prize.
Your ticket automatically enters you into a prize draw to win one of dozens of prizes including tickets to Kew Gardens, a tour of Fuller’s brewery, a cut & blow at a Headmasters salon nationwide, a Benefit make-up set, cupcakes from Beas of Bloomsbury and many more!
16
TUESDAY
TH DECEMBER
17:30-24:00
Raffle tickets will be available for £2 each if you can’t make the pub crawl
SCHEDULE: 17:30 18:30 - 19:15 19:15 21:30 - 23:30 24:00
it Adm One
Depart from office Drinks reception Sit down for dinner DJ Finish
Dress code: formal & fabulous (no jeans or trainers) The White Horse
The Duke
Worple Way, Richmond Surrey, TW10 6DF
2 Duke Street, Richmond Surrey, TW9 1HP
TABLE NO:
Tommy’s
Tickets £5 in advance
YOU!
presents
The Slug and Lettuce Riverside House, Water Lane Richmond, Surrey, TW9 1TJ
Pitcher & Piano 11 Bridge Street, Richmond, Surrey, TW9 1TQ
www.tommys.org
To be in with a chance of winning make a donation to Tommy's - the premature and stillbirth baby charity and guess my finish time for cycling the 100 miles
WIN
WIN WIN
100 moriles
Name
CLOSEST
t Second Third Firs Prize Prize Prize
GUESS WINS... £25 £15 Contact
Finish Time
Donation
£5 Paid
F
COME SUPPORT US
Andrew and King will be cycling 100 miles as part of the Ride London challenge to raise money for
Tommy's - the premature and stillbirth baby charity.
Currently, 1 in 4 women lose a baby during pregnancy and labour - we want to see this change. Please help us by making a donation to support Tommy's research, and we'll take on the 100 miles of leg-testing climbs through London and into the Surrey countryside. Thanks for all your support!
Ross Wilson
Andrew and King
uk.virginmoneygiving.com/team/CrestonHealth-RideLondon 100 mForiles
www.tommys.org
www.tommys.org
Training Holiday Entitlement
Health and Lifestyle
We offer better than average annual leave, including a loyalty scheme .
Your health matters to us Company pension, healthcare benefits that extend to include your children, and other great perks.
The Little Book of Big Benefits
Healthshield Instant cashback to help cover the cost of everyday healthcare needs including £110 cashback p/a on dental & optical & £290 on physio. Access to a 24/7 counselling and support helpline.
3% contributory Company pension On successful completion of your probation period, we offer a matching contributory pension of 3% of your salary.
Group Life Assurance plan through ‘MetLife’ Our life insurance scheme pays out a lump sum of 4 x your annual salary.
There are lots of lovely ways to make more of your time at Health Unlimited.
25 days
Additional days
This is 25 days each year, which runs from 1st January to 31st December, plus all UK bank holidays. This gets prorated to your start date in your first year and is adjusted according to your working pattern if you work part time. We also give you:
More annual leave for your loyalty, starting with an extra 1.5 days after 3 years’ service, with an additional half day for every completed year of employment up to a total allowance of 30 days thereafter.
Take a look.
Giving back Wherever possible, we try to encourage support of local and international charities
Tastecard Discounted annual tastecard (corporate rate) will give you great discount deals at over 6,500 restaurants nationwide including PizzaExpress, STRADA, La Tasca, Prezzo and Zizzi.
Carnaby Privilege Card Carnaby Privilege Card Anyone who lives or works within Carnaby or Soho is eligible for a Neighbourhood Card. Offering you a 10% discount at participating shops, cafés, restaurants, bars and clubs in and around Carnaby Street, including Liberty, Office, Benefit, Flat Iron, Pizza Pilgrims and many more. In addition, you can enjoy exclusive promotions and invites to launches and events.
PROJECT
WORK TYPE
Invites & events design and development
Print and digital media
Annual Charity Day To enable you to support the charity of your choice with your own time
S Ku
CLIENT
Abbott NOW APPROVED FOR AGES 4-17*
FREE TO
DREAM WITHOUT LANCETS
†
NEW! Introducing the FREE LibreLink App1 Taking breakthrough technology a step further
Patients can now scan their FreeStyle Libre sensor using the free LibreLink app on their Android smartphone2,3
Welcome to flash glucose monitoring.
The LibreLink app makes it easier for your patients to check their glucose anytime, anywhere.
With the FreeStyle Libre system, you and your child can check glucose without routine finger pricks.‡
Why prick, when you can scan?4
Why prick, when you can scan?‡
FREE app download:
Find out more at www.FreeStyleLibre.com *A caregiver at least 18 years old is responsible for supervising, managing, and assisting the child in using the FreeStyle Libre system and interpreting its readings. Scanning the sensor does not require lancets. ‡ A finger prick test using a blood glucose meter is required during times of rapidly changing glucose levels when interstitial fluid glucose levels may not accurately reflect blood glucose levels or if hypoglycaemia or impending hypoglycaemia is reported by the System or when symptoms do not match the System readings. †
Information contained herein for distribution outside of the US ONLY. Local legal and regulatory approval is required to publish any content. FreeStyle and related brand marks are trademarks of Abbott Diabetes Care, Inc. in various jurisdictions. © 2015 Abbott DOC37018_Rev-B
1 The LibreLink app includes a mobile application, provided by AirStrip, and data management services, provided by NewYu, Inc. Registration with NewYu, Inc. is required during app setup. Abbott, provider of the FreeStyle Libre readers and sensors, is not the provider of the LibreLink app. 2The LibreLink app is compatible with NFC-enabled smartphones running Android OS 4.0 or higher. | 3When a FreeStyle Libre sensor is started with the LibreLink app, it is linked exclusively to the app and that smartphone. Once linked, a FreeStyle Libre reader or other LibreLink account cannot be used to scan that sensor. | 4A finger prick test using a blood glucose meter is required during times of rapidly changing glucose levels when interstitial fluid glucose levels may not accurately reflect blood glucose levels or if hypoglycaemia or impending hypoglycaemia is reported by the LibreLink app or when symptoms do not match the LibreLink app readings. | Airstrip Technologies develops and maintains the LibreLink app. | NewYu, Inc. is the exclusive provider of data management services for the LibreLink app. | FreeStyle and related brand marks are trademarks of Abbott Diabetes Care Inc. in various jurisdictions. Other trademarks are the property of their respective owners. | DOC35729 Rev. C 09/15
11/15
Finger pricking is a big source of stress for children with diabetes
Children undergo finger-prick testing on average six times a day and dislike it for many reasons including hassle and pain*
6
Times/Day
FREE TO
PLAY
WITHOUT LANCETS*
Parents believe diabetes restricts their child’s life
51% suffer sleep disruption due to diabetes management*
FLASH GLUCOSE MONITORING SYSTEM
44% say measuring glucose levels is the biggest source of interruption for their child*
* Survey of 600 parents of children aged 4 – 14 years with type 1 diabetes. Conducted by Opinion Health January 2016
5
6
7
8
Upload Data
View Reports
Create a Practice
Manage Your Patients
Follow on-screen instructions to upload your patients’ reports
One easy view for consistent reports in one place
You can… • Customise report settings for individual patients OR all patients in your practice TIP
If your patients use the LibreLink app, their diabetes information will sync to LibreView without the need for cables
• Customise the report criteria and the types of report that are generated each time
Invite patients to share glucose data from home and invite colleagues to view the same patient data you see
• Open the menu in • Enter your practice LibreView and click information and “Create a LibreView click “Create Practice” Practice”
Front
The ‘My Patients’ dashboard
Quick Start Guide for Healthcare Professionals
Use the dashboard to identify patients and access saved reports
Flag patients to keep track of the ones that may need more attention
• Compare glucose history for each patient
CLIENT
PROJECT
WORK TYPE
Abbott
FreeStyle Libre marketing material
• Editorial Layouts • Social Media Content • Gifs • E-Marketing Designs
63% report their child having had at least one episode of severe hypoglycaemia during sleep*
• PowerPoint Presentations • Website Design • Infographics
All your patients’ glucose data in one secure, cloud-based location
CLIENT
Abbott Wednesday 18th February
CLINICAL UTILISATION OF THE FREESTYLE LIBRE SYSTEM
2015
TECHNICAL AND CLINICAL ADVANCES IN FLASH GLUCOSE MONITORING
Monday 1st October
2018
Abbott Diabetes Care Industry Symposium
16:45 — 18:15hrs
The first 14-day, no calibration sensor-based flash glucose monitoring system
CNIT
2 Place de la Défense 92053 La Défense France
FreeStyle Libre System Accuracy Study Timothy S. Bailey, MD
14:30 – 17:00
Please register with EASD in advance for this symposium.
Rapoport Hall
Industry symposium supported by Abbott on the occasion of the 54th Annual Meeting of the European Association for the Study of Diabetes.
Messedamm 22 14055 Berlin Germany
Improving Patient Outcomes with Constructive and Meaningful Dialogue using Ambulatory Glucose Profile Iain Cranston, MD Using the FreeStyle Libre System and Ambulatory Glucose Profile to Uncover Glucose Information in Patients with Type 1 Diabetes Jean-Pierre Riveline, MD Panel Discussion Professor Cliff Bailey and all Presenters
FreeStyle and related brand marks are trademarks of Abbott Diabetes Care, Inc. in various jurisdictions. ADC-EM2018FSL008
TECHNICAL AND CLINICAL ADVANCES IN FLASH GLUCOSE MONITORING
XXXXDAY XXTH AUGUST
2019 14:30 – 17:00
ABBOTT DIABETES CARE INDUSTRY SYMPOSIUM
VENUE BARCELONA
Industry symposium supported by Abbott on the occasion of the 55th Annual Meeting of the European Association for the Study of Diabetes. FreeStyle and related brand marks are trademarks of Abbott Diabetes Care, Inc. in various jurisdictions. ADC-XX2019FSL000
NE W !
CLINICAL UTILISATION OF THE FREESTYLE LIBRE SYSTEM
FLASH GLUCOSE MONITORING
The first 14-day, no calibration sensor-based flash glucose monitoring system
Clinical Use from Childhood through Adulthood Industry symposium supported by Abbott on the occasion of the International Conference on Advanced Technologies & Treatments for Diabetes (ATTD) 2016
Wednesday 18th February 2015, 16:45—18:15hrs PROGRAMME EVALUATION FORM Your feedback on this symposium is very important to us; please take the time to answer the following questions, and leave your completed form on your seat or hand to a member of the symposium staff.
Session Evaluation Please rate each of today’s presentations where 1=poor and 5=excellent
1
2
3
4
5
FreeStyle Libre System Accuracy Study Timothy S. Bailey, MD Improving Patient Outcomes with Constructive and Meaningful Dialogue using Ambulatory Glucose Profile Iain Cranston, MD Using FreeStyle Libre System and Ambulatory Glucose Profile to Uncover Glucose Information in Patients with Type 1 Diabetes Jean-Pierre Riveline, MD
Welcome to Flash Glucose Monitoring.
Panel Discussion Professor Cliff Bailey and all Presenters
The days of routine glucose testing with lancets, test strips and blood are over.†
Overall Evaluation
WHY PRICK, WHEN YOU CAN SCAN?†
Will the information you have heard here change your practice in the future?
Yes
Maybe
Yes Maybe
No
No
Would you like to hear more about AGP?
To find out more, visit us at Stand #3 during the ATTD AbbottNextFrontier.com
If yes, how:
Yes
Maybe
Wednesday 3 February, 14:30 – 16:00 Hall C - Blue Hall Chair of the Symposium: Professor Emanuele Bosi, M.D. Vita-Salute San Raffaele University, Milan, Italy XX:XX – XX:XX
First Clinical Experience with FreeStyle Libre in Young Adults and Children with Type 1 Diabetes Fiona M Campbell, M.D. Leeds Teaching Hospitals Trust, UK
XX:XX – XX:XX
Clinical Use of FreeStyle Libre in Adults with Type 1 Diabetes Professor Emanuele Bosi, M.D. Vita-Salute San Raffaele University, Milan, Italy
XX:XX – XX:XX
Use of FreeStyle Libre in Intensively Managed Adults with Type 2 Diabetes Gerry Rayman, M.D. Head of Service, Diabetes Care, Ipswich Hospital NHS Trust, UK
XX:XX – XX:XX
Panel Discussion Professor Emanuele Bosi, M.D. and all presenters
No
Would you like to hear more about Flash Glucose Monitoring?
What topics related to sensor technology would you find interesting at future satellite symposia?
* Scanning the sensor does not require lancets. †
A finger prick test using a blood glucose meter is required during times of rapidly changing glucose levels when interstitial fluid glucose levels may not accurately reflect blood glucose levels or if hypoglycaemia or impending hypoglycaemia is reported by the System or when symptoms do not match the System readings. FreeStyle and related brand marks are trademarks of Abbott Diabetes Care Inc. in various jurisdictions. Simulated data for illustrative purposes only; not real patient or data. Date of preparation: August 2014. ADCMDP140136r
‡
FreeStyle Libre is currently only available via purchase from Abbott Diabetes Care
To find out more about FreeStyle Libre go to www.AbbottNextFrontier.com FreeStyle and related brand marks are trademarks of Abbott Diabetes Care, Inc. in various jurisdictions.© 2015 Abbott ADC/ATTD2015/013
CLIENT
PROJECT
WORK TYPE
Abbott
FreeStyle Libre marketing material
• Editorial Layouts • Social Media Content • Gifs • E-Marketing Designs
• PowerPoint Presentations • Website Design • Infographics
FreeStyle and related brand marks are trademarks of Abbott Diabetes Care, Inc. in various jurisdictions. ADC/ATTD2016/008
CLIENT
Amgen YOUR E V I G ENTS’ PATI E HEALTH BON T TER A BE NCE CHA Are your patients at risk of fragility fractures?
YOUR GIVEES A BONNING WIN NCE CHA Healthy bones help you stay active and do the things you love. TALK TO YOUR DOCTOR ABOUT YOUR OSTEOPOROSIS RISK CHECK RESULTS
Book your doctor’s appointment Date
WHAT IS OSTEOPOROSIS?
Time
Osteoporosis reduces the density of your bones. This can make your bones more fragile which can lead to fractures. Bone loss occurs without you knowing, and often without symptoms until a fracture happens. You can discuss your risk and treatment options with your doctor.
QUESTIONS TO ASK YOUR DOCTOR 1. Am I at risk of osteoporosis? 2. Do I need a bone density scan?
Osteoporosis makes your bones more fragile as you age which can lead to fractures. Keep your bones healthy and do the things you love for longer.
WHAT IS A BONE DENSITY SCAN?
3. What can I do to improve my bone health?
A bone density scan, often referred to as a DEXA scan, measures your bone strength and helps your doctor make a diagnosis. It only takes 10 to 20 minutes, depending on which part of your body is being scanned. It is completely painless. You can ask your doctor to describe the procedure to you.
4. Other questions
RAISING AWARENESS OF RISK FACTORS FOR OSTEOPOROSIS
GIVER YOU ES BON NNING A W IN C E CHA
CHECKLIST
Print and bring my Osteoporosis Risk Check results Note any medication or supplements
Take the 1 minute test and talk to your doctor.
ILE FRAG S .EU E N O B
In collaboration with insert local P.A.G logo here
© 2020 Amgen Inc. All rights reserved. EUHQ-P-162-0120-081363b March 2020
This initiative is supported by
ST? BONE TE
THE WHAT ISOROSIS OSTEOP HECK? C K IS R
THE GAME OF NCE CHA
YOUR GIVE NTS’ BONE PATIE H A BETTER HEALT CE CHAN
In collaboration with insert local P.A.G logo here
Developed by the International Osteoporosis Foundation (IOF), this eight-question risk check for older women identifies key risk factors for osteoporosis.
Q1 Q2 Q3
The Spanish Foundation for Osteoporosis and Metabolic Bone Diseases (FHOEMO) is launching a communications campaign on [date] to help women 65 years and over in Spain become more aware of their risk of fragility fractures.
Q4 Q5 Q6 The Game of Chance campaign encourages older women to take The Osteoporosis Risk Check to raise their awareness of osteoporosis risk factors. If results of the risk check are positive, women are encouraged to discuss their risk of osteoporosis with their doctor.
Q7 Q8
Are you aged 60 or older? Have you broken a bone after the age of 50? Are you underweight?
Are they at risk of fragility fractures?
Body Mass Index
After the age of 40, have you lost more than 4cm in height (ca. 1.5in)? Have either of your parents had a hip fracture? Do you have any of the following disorders? Rheumatoid arthritis ∞ Digestive tract diseases ∞ Prostate or breast cancer ∞ Diabetes ∞ Chronic kidney disease ∞ Thyroid gland disorders ∞ Lung disorder ∞ Low testosterone ∞ Early menopause, periods stopped, or ovaries removed ∞ Immobility ∞ HIV
Have you been treated with any of the following medications? Glucocorticoids ∞ Aromatase inhibitors ∞ Androgen deprivation therapy ∞ Thiazolidinediones ∞ Proton pump inhibitors ∞ Thyroid hormone treatment ∞ Immunosuppressants ∞ Antidepressants ∞ Steroid hormones ∞ Antipsychotics ∞ Anticonvulsant
Do you drink excessive amounts of alcohol (more than 3 units a day) and/or currently smoke?
The IOF Osteoporosis Risk Check (#IOFRiskCheck) is intended as a tool to raise awareness of factors which are known to increase the risk of osteoporosis and fractures. This awareness tool has been reviewed and approved by IOF’s Committee of Scientific Advisors. The IOF Osteoporosis Risk Check is not a diagnostic tool: only a doctor can diagnose osteoporosis. An interactive version of the risk check is available on the International Osteoporosis Foundation website http://riskcheck.iofbonehealth.org
In collaboration with insert local P.A.G logo here
This initiative is supported by AMGEN Europe GmbH Suurstoffi 22, P.O. Box 94, CH-6343 Rotkreuz, Switzerland
© 2020 Amgen Inc. All rights reserved. EUHQ-P-162-0120-081363c March 2020
ILIT Y FRAGTURES FRAC E T V HA IMPAC A BIGIVES ON L
ILIT Y FRAGTURES FRACMORE AN E AR MON TH COMMIGHT YOU K THIN ?
1
+
+28.
8%
≥ 330,000
Fragility fractures affect more women than stroke, breast cancer and cardiovascular disease combined.
4
One year after a hip fracture 63% of patients have limitations on daily tasks such as driving, shopping, walking unaided, using the toilet and taking a shower.
US HELPSE THE CLO NOSIS G DIA GAP
Women over 65 years with a previous fragility fracture are recommended for treatment. Recognising clinical risk factors to assess probability of fractures can direct management decisions to prevent fractures.
?
3 in 4 patients at risk of fragility fractures were not receiving osteoporosis medication.
420,000
+ 3
?
2
1 in 2 patients over 75 years visiting their primary care physician were at increased risk of fragility fractures.
This initiative is supported by
2017
2030
NTS PATIEE THEIR E VALUPENDENC INDE TIVE LIFE & ACVE ALL ABO
1
Prior fragility fracture
2
Advanced age (65 years +)
3
Parental history of hip fracture
20% 80%
In a survey of women 75 years and under, 80% would rather be dead than have to enter a nursing home due to loss of independence after a hip fracture.
4
History of falls
5
Glucocorticoid treatment
Incidence of fragility fractures in Spain is increasing every year.
CLIENT
PROJECT
WORK TYPE
Amgen
‘Give your Bones a Winning Chance’
• Editorial Layouts • Social Media Content • Gifs
The 1 Minute Test is not designed to assess absolute risk. Please use FRAX®,DXA or other validated clinical diagnostic tools to further assess at-risk patients.
• New Business Visualisations • E-Marketing Designs • Infographics
CLIENT
Almirall Do you know the ABC of IBS? About IBS People with IBS experience bouts of:1
IBS is a chronic,
relapsing and often lifelong disorder, characterised by abdominal pain and/or discomfort, bloating and changes in bowel habit1
IBS is common in
Scotland with a
prevalence in adults of 7.7% for those who seek medical help2
Only half
of those with IBS symptoms present to their primary care physician1
Almirall IBS Timeline
Do you know your Irritable Bowel Syndrome sub-types? IBS-C
IBS-D
Lots of stomach pain, bloating and change in
7.7%
A
Irritable Bowel Syndrome with CONSTIPATION - IBS-C
Abdominal pain
B Bloating
C
IBS
has a significant impact on both patients 3 QoL and the healthcare resource use4
Almost twice as common in women than men2
IBS
IBS-M
half
Almost of IBS patients in Scotland are treated with prescription medication2
One-third of patients with IBS are thought to have IBS-C2 which means they suffer chronically from both abdominal pain and constipation.
bowel habits – give it a week or so before thinking it’s not just a stomach bug…
– there’s some scary stuff out there! Could it be cancer? There’s lots of information but I’m still not sure what it could be.
GP tells me it’s nothing, I just need to watch what I eat. I feel like I’ve wasted her time
Irritable Bowel Syndrome with DIARRHOEA - IBS-D One-third of patients with IBS are thought to have IBS-D2 which means they suffer chronically from both abdominal pain and diarrhoea.
Change in bowel habits
Do some online research
Have been Googling. I could have something
called IBS – my symptoms do seem to match those being described. It’s a relief that it’s not cancer but I still don’t feel well and it’s now been months since my symptoms first appeared. Want to go back to my GP but not sure she can help as she didn’t last time.
3x
Irritable Bowel Syndrome MIXED - IBS-M One-third of patients with IBS are thought to have IBS-M2 which means they suffer chronically from abdominal pain and both constipation and diarrhoea.
Additional information For further information, or to discuss your case study needs, please contact Abigail Thomson or Caroline Howley using the contact details:
Up to 50%
of referrals to gastro for IBS are perceived to be wasteful of specialist resources5
IBS cannot be cured1 and treatment focuses on symptom control.
multiple treatment
Often
approaches may be required.1 Abigail Thomson athomson@rdcomms.com 020 8392 8049
Caroline Howley chowley@rdcomms.com 020 8392 6938
50%
less than 25% of patients report complete relief of any one of their IBS-C symptoms6
Feel isolated as I don’t really
References: 1. NICE. Clinical Practice Guideline: IBS in adults. 2008 2. Information Services Division. An investigation into the prevalence, management and healthcare burden of irritable bowel syndrome in Scotland.2012 3. Spiller R, et al. Guidelines on the irritable bowel syndrome: mechanisms and practical management Gut 2007;56:1770-98 4. Cash B, Sullivan S, Barghout V. Am J Manag Care. 2005; 11(1 Suppl): S7-16
1 2
With existing treatments,
3
5.
British Society of Gastroenterology. IBS functional symptoms - BSG commissioning report. Available at http://www.bsg.org.uk/images/Commissioning_report/BSG_ IBS_and_Functional_symptons.pdf [Accessed March 2013]
6.
Hungin APS et al. The prevalence, patterns and impact of irritable bowel syndrome: an international survey of 40,000 subjects. Aliment Pharmacol Ther 2003;17:643–650
want to talk to my friends and family about my bowel habits and how the change in them, and the other symptoms like pain and bloating, are affecting me – have tried some over the counter things but nothing seems to work. I also feel that I’m constantly moaning about not feeling well and have even had to take a few days off work.
I found a useful resource on a patient website – it’s a
simple three question questionnaire that indicates whether or not I have IBS – seems like I do. Going to take the results to my GP and see if a diagnosis can be made…
Date of preparation: April 2013 Job number: UKLIN1826b
CLIENT
PROJECT
WORK TYPE
Almirall
Various marketing material
• • •
Editorial Layouts Social Media Content Website Design
• Infographics • Exhibition
Bite the bullet and visit my GP again as feel so rotten – feel more informed and
confident though since taking the online questionnaire. I ask to see a different GP to last time and really run through my symptoms. Much more positive experience! I now have a diagnosis and feel so relieved that I definitely know what’s wrong and that it is manageable.
Hooray! After being careful with my diet and really knowing what triggers my symptoms, I feel so much more in control of my body and my life. I’m able to socialise more without worrying about an IBS attack and my friends at work have noticed a difference too – I can’t stress enough how important it is for people to keep researching and seeking help from their GP. My life is now mine again. My IBS, my life.
CLIENT
Takeda - Alunbrig
Explore two real-life ALUNBRIG patient experiences alongside relevant efficacy and safety data Read Tom’s case
Read Susan’s case
A 60-year-old chef who has ALK+ aNSCLC that has progressed with CNS involvement after front-line therapy and is experiencing neurological symptoms.
A 73-year-old retired journalist with osteoarthritis, osteoporosis and hypothyroidism and chronic musculoskeletal pain.
Explore Tom’s experience of ALUNBRIG and the relevant supporting clinical data.
Explore Susan’s experience of ALUNBRIG after progressing with front-line therapy for ALK+ aNSCLC.
ALUNBRIG® (brigatinib) is indicated as monotherapy for the treatment of adult patients with anaplastic lymphoma kinase (ALK)-positive advanced non-small cell lung cancer (aNSCLC) previously treated with crizotinib.1
References 1. ALUNBRIG Summary of Product Characteristics.
January 2019 UK/BRIG/1810/0029k
Not for further copying or distribution
PI
EFFICACY | TOLERABILITY | DOSING | SUMMARY | GLOSSARY
PI
EFFICACY | TOLERABILITY | DOSING | SUMMARY | GLOSSARY
Click tabs to explore key ALUNBRIG data at any point. Use the arrows to work through the case study.
Tom’s treatment history
Crizotinib initiated
Grade 2 fatigue Grade 2 nausea
Intracranial protection extending out to one and a half yearsa,1-4
Developed CNS symptoms: unsteadiness dysarthria, vertigo and nausea Following progression on crizotinib, Tom commenced ALUNBRIG at 90 mg/day
OCT 2015
DEC 2015
Pemetrexed + cisplatin
Chemotherapy discontinued (after cycle 3)
JAN 2016
APR 2017 Discontinued crizotinib after 15 cycles
MRI: New, extensive CNS involvement (subtle leptomeningeal disease)
IRC-assessed intracranial PFSb in patients with any brain metastases at baseline1
Reviewed at 7 days, no worsening of neurological symptoms, no toxicities of treatment, so dose was escalated to 180 mg/day
Treatment goal • Palliative, aiming for improved quality of life
Adapted from Huber MH, et al. 20181
Intracranial mDOR (IRC assessed) of 16.6 months (95% CI 3.7-NR) in patients with measurable brain metastases at baseline.2-4 a
Why ALUNBRIG?
In patients with brain metastases at baseline. bIntracranial PFS does not include systemic (non-cranial) disease progression events. 180 mg once daily with 7-day lead-in at 90 mg once daily.
c
• PFS data from the ALTA study • As Tom works in food preparation, GI toxicity was an important consideration References 1. Huber RM, et al. Poster presentation at ASCO Annual Meeting 2018, Poster 384; 2. Camidge DR, et al. J Clin Oncol 2018;36:2693-2701; 3. Ahn M-J, et al. Oral presentation at IASLC 18th World Conference on Lung Cancer, 2017; 4. Ou S-HI, et al. Oral presentation at ESMO 2017, poster 1345P.
Not for further copying or distribution
Not for further copying or distribution
ALTA: evaluating the efficacy and safety of ALUNBRIG
Raising expectations in
ALK in Lung Cancer Trial of AP26113 (ALTA): a phase 2, global, randomised, open-label, multicentre trial. Objective: to assess the efficacy and safety of two ALUNBRIG dosing regimens.
ALK+ aNSCLC post crizotinib Exceeds 1 year median PFSa in ALK+ aNSCLC patients post crizotinib1
LICENSED INDICATION
ALTA was not a controlled trial and not designed for statistical comparisons between dosing regimens.
ALUNBRIG® (brigatinib) is indicated as monotherapy for the treatment of adult patients with anaplastic lymphoma kinase (ALK)-positive advanced non-small cell lung cancer (aNSCLC) previously treated with crizotinib1
Primary endpoint was confirmed ORR according to Response Evaluation Criteria In Solid Tumors (RECIST v1.1) as evaluated by investigator. a
a IRC and investigator assessed. UK/BRI/1807/0001 Date of preparation: January 2019
CLIENT
PROJECT
WORK TYPE
Alunbrig
Isell detail aid
• E-Marketing Designs
Patients in the 90 mg arm were allowed to escalate to 180 mg after RECIST progression.
ye drop nctivitis Dosage p to be at least nsitivity ons and ystalline Contains known eported nded or istance. eriences devoid nancy if infants effects: of the ing and various ensation ts at the ritation, vision. mation) o fusidic o cause stitute a 7.57 per arketing Co), 1st Date of
ority.
orted
.com.
ary 2016
CLIENT
AMCo
Efficacy
Key facts about
Tolerability
Fucithalmic® has a proven comparable efficacy profile, as efficacious as tobramycin, chloramphenicol and norfloxacin1-3
A guide for healthcare professionals
Fucithalmic® is a well tolerated treatment with mild and transient adverse events7 Fucithalmic® is a preferred treatment option for pregnant women where benefit outweighs risk (NICE, UK health guidance body)8
Fucithalmic® has a sustained targeted action against the most common pathogens causing bacterial eye infections, namely streptococcus pneumoniae, staphylococcus aureus and haemophilus influenzae4,5
This leaflet tells you all you need to know about Fucithalmic® eye drops, an effective treatment option for the most common bacterial eye infections
Fucithalmic® offers low discontinuation rates9
Formulation
Convenience
Fucithalmic® is administered as a viscous eye drop easing application for patients of all ages and causes less blurring compared to an ointment1
Fucithalmic® is an effective and convenient twice daily treatment option2 Unique carbomer gel formulation prolongs contact time with the eye for up to 12 hours6
References 1. Normann EK, et al. Acta Ophthalmol Scand. 2002;80:183–87. 2. Jackson WB, et al. Can J Ophthalmol. 2002;37:228–237. 3. Wall AR, et al. J Clin Res. 1998;1:316–325. 4. Arrata M. Acta XXV Concilium Ophthalmologicum. 1987;1038-1042. 5. Morrow GL, et al. Am Fam Physician. 1998 Feb 15;57:4:735-46. 6. van Bijsterveld OP, Andriesse H, Nielsen BH. Eur J Drug Metab Pharmacokinet. 1987 Jul-Sep;12:3:215-8. 7. Hvidberg Jesper. Acta Ophthalmol. 1987;65:43-47. 8. NICE. Clinical Knowledge Summaries. Conjunctivitis – infective. 2015. Available from: cks.nice.org.uk/conjunctivitis-infective (accessed December 2015). 9. Sinclair NM. Curr Ther Res. 1988;44:468-73.
Fucithalmic® is a patient friendly treatment, with 91% of patients fully compliant3
Prescribing information is included at the end of this guide Initiated, funded and reviewed by AMCo/FUT/1215/0029a
Date of preparation: February 2016
BACTERIAL CONJUNCTIVITIS CONSULTATIONS
Initiated, funded and reviewed by AMCo
BACTERIAL CONJUNCTIVITIS CONSULTATIONS
Initiated, funded and reviewed by AMCo
Talking about bacterial conjunctivitis
Bacterial conjunctivitis and your patients
Conversation starters – getting the most out of your patients
If antibiotic treatment is required, encourage patient to elaborate on the below to prescribe a suitable topical eye ointment or eye drops
BACTERIAL CONJUNCTIVITIS CONSULTATIONS
Initiated, funded and reviewed by AMCo
Bacterial Conjunctivitis What is it and why do I have it? Bacterial conjunctivitis (or ‘red eye’) is a condition that causes redness and swelling of the thin layer of tissue that covers the inside of the eyelids and front of the eye – the conjunctiva. It can be easily spread by direct or indirect contact with others who are infected.
The low down on bacterial conjunctivitis
Estimated to comprise 1% of all consultations in primary care1
Leading cause of absenteeism from nursery, school and work2
Represents approximately 40% of ocular diagnoses in children3
1%
Tips to get your patients talking about bacterial conjunctivitis
PAGE 1
A
Symptoms
B
Aetiology
Ask patient / care giver to describe symptoms and prompt to articulate duration and severity of the condition
Infectious or non-infectious? Probe to determine the most likely cause of the symptoms and identify any known risk factors
C
Self-treatment to date
D
Impact
Impact on attendance at school or work? Question to uncover the full impact of the condition on the patient’s / care giver’s day-today life
Proper care and treatment adherence are essential for speedy recovery. Some tips are provided in the accompanying take-away patient guide to reinforce any advice given during the consultation
Job Code: GL/FUC/RDP/997A/2015 | Date of preparation: November 2015
Nature of condition and how treatment may support quicker resolution of symptoms
Explore patient understanding of contagious nature of condition and provide information on how antibiotics may help to avoid spread of infection4
B
Lifestyle of patient or care giver
C
Treatment application
Confirm self-care measures to date and what has / hasn’t helped to relieve symptoms
Beyond the consultation: patient education
Here are some suggestions to support your consultations and patient dialogue
A
Probe to understand importance of treatment convenience for the patient / care giver, to support faster recovery and better compliance with fewer applications
Determine patient / care giver preferences regarding treatment application. Depending on the patient's agreement, prescribe a suitable treatment
Patient education is very important to stop the spread of infection and speed up the resolution of symptoms
Why not share the accompanying patient advice sheet at the end of your consultation? It contains some useful care advice to support patient compliance in the treatment of bacterial conjunctivitis
References 1. Høvding G. Acta Ophthalmol 2008;86:5–17. 2. Rose PW, Ziebland S, Harnden A, et al. Fam Pract 2006;23:226–32. 3. Gold RS. Pediatric Annals 2011;40:95–105. 4. Smith AF, Waycaster C. BMC Ophthalmology 2009;9:13.
PAGE 2
Job Code: GL/FUC/RDP/997A/2015 | Date of preparation: November 2015
CLIENT
PROJECT
WORK TYPE
AMCo
Various marketing material
• Editorial Layouts • New Business Visualisations • Infographics
Not only is bacterial conjunctivitis highly infectious, it can also be very uncomfortable.
Here are some pointers to help ease any discomfort and to prevent spreading the condition to others. Care tips
Prevent the spread of bacterial conjunctivitis
Always use medication as directed – just speak to your HCP if you have any questions
Keep face flannel, towel and pillow separate from those of the rest of the family
Clean away any discharge from eyelids and lashes using cotton wool soaked in cooled boiled water
Wash your hands thoroughly and regularly, particularly after touching your eyes
Do not wear contact lenses until the conjunctivitis has cleared up
Use tissues if you need to wipe your eyes and dispose of them immediately afterwards
Under no circumstances allow anyone else to use your eye ointment or drops. Throw them away when your treatment is finished. Never keep used bottles
Don’t go swimming at public swimming pools until your infection is completely treated
PAGE 1
Job Code: GL/FUC/RDP/997A/2015 | Date of preparation: November 2015
CLIENT
Astellas Spotlight In the
Integrity
Action
Spotlight In the
Rochelle and Daniel
in
Take responsibility . Act ethically . Lead by exampl e.
NAME OF PERSON
What are the outputs?
In the first of our new In The Spotlight series, we heard from Rochelle Chopamba and Daniel Schulze. They introduced us to the world of HR and legal and shared with us how they interact on a day-to-day basis. Part of their cross-functional role involves sitting on the Case Review Committee, which they tell us about in their video.
Integrity
Action
in
Take responsibility. Act ethically. Lead by example.
Jan 2017
For those interested in understanding more about the Case Review Committee (CRC) and what happens when you speakup, outlined below is the CRC Charter.
• Agreement on identity of investigation lead and investigation support
If you have any questions about speaking-up or this Charter, please feel free to speak to Rochelle, Daniel or their colleagues in HR/legal.
• Agreement on next steps and corrective actions if required following completion of investigation and review of the subsequent report
Welcome to the In the Spotlight newsletter. Lorem ipsum dolor sit amet, consectetur adipiscing elit. Vivamus finibus massa erat, sed condimentum justo tincidunt in. Curabitur non odio nec urna fringilla luctus. Proin vitae dui ut nisi vehicula mattis non ac felis. Pellentesque habitant morbi tristique senectus et netus et malesuada fames ac turpis egestas. Pellentesque convallis euismod risus, sit amet interdum risus varius vel. Vestibulum id ligula faucibus, dictum purus in, condimentum dui. Donec iaculis varius erat, ac fermentum libero. Aliquam hendrerit sit amet nisi in aliquet. Maecenas faucibus lacinia massa id rutrum. Donec pharetra nisl id tincidunt pellentesque. Nullam ut vehicula dolor, ut ornare nulla.
• Agreement on lessons learned and appropriate training to EMT/HLT/affiliates when deemed necessaryappropriate
What is the purpose of the CRC? The Case Review Committee (CRC) review all reports received on a case by case basis to ensure that it is triaged to the appropriate leadership and function for investigation and resolution.
Purpose
The CRC consider whether any case received warrants disclosure to an external regulator.
The Case Review Committee (CRC) to review all reports received on a case by case basis to ensure that it is triaged to the appropriate leadership and function for Investigation and resolution.
The CRC review the outcome of the investigation and challenge/ review the steps taken and make appropriate recommendations.
The CRC to consider whether any case received warrants disclosure to an external regulator. The CRC to review the outcome of the investigation and challenge/review the steps taken and make appropriate recommendations.
Why is the CRC important? Senior leadership must demonstrate that all reports received are treated with utmost seriousness and are assigned to the appropriate function to ensure that allegations are fully investigated and outcomes are appropriately reviewed and challenged.
Importance
Two of the following are required to confirm the CRC is quorate and 1 of Head of Ethics and Compliance or General Counsel EMEA:
What input goes into the CRC? • Initial case report details
Senior leadership must demonstrate that all reports received are treated with utmost seriousness and are assigned to appropriate function to ensure that allegations are fully investigated and outcomes are appropriately reviewed and challenged.
• Head of Ethics and Compliance EMEA (Chair)
• Any expert insight as appropriate
Inputs
• President of EMEA Operations, EMEA or delegate
• Investigation report and proposed next steps/corrective actions
• Initial case report details • Any expert insight as appropriate
• General Counsel EMEA
What process do the CRC follow?
• Investigation report and proposed next steps / corrective actions
• VP, HR or delegate
• Head of Ethics & Compliance EMEA to introduce the case and chair the discussion on how to proceed
N.B. Should one of the above attendees be identified in the case report, they will be excluded from any decision related to that case
• All to advise of any legal, HR or business implications • All to consider if a disclosure to an external regulator is required
Process • Head of Ethics & Compliance EMEA to introduce the case and chair the discussion on how to proceed
• Review of output of the investigation to ensure proposed next steps and corrective actions are appropriate
• All to advise of any legal, HR or business implications • All to consider if a disclosure to an external regulator is required • Review of output of the investigation to ensure proposed next steps and corrective actions are appropriate
Outputs • Agreement on identity of investigation lead and investigation support • Agreement on next steps and corrective actions if required following completion of investigation and review of the subsequent report • Agreement on lessons learned and appropriate training to EMT/HLT / Affiliates when deemed necessary
Astellas Communications Network Map
2 of the following is required to confirm the CRC is quorate and 1 of Map Astellas Communications Network Head of Ethics and Compliance or General Counsel EMEA: EMEA TEAM:
AFFILIATES:
AFFILIATES:
• Head of Ethics and Compliance EMEA (Chair) Christina Chale (EMEA)
Stefan Bevers
• President of EMEA Operations, (The Netherlands)EMEA or delegate
Interim Corporate Communications Director
AFFILIATES: Vadim Kurenkov (Russia & CIS) Head of Recruitment, Personnel Development & HR Communications
• General Counsel EMEA
Jan Milton-Edwards (EMEA)
• VP, HR or delegate
Corporate Communications Director
Louise Carmén (Nordic & Baltic Operations) Communication & Commercial
Antonella Di Lorenzo (Italy) Communications, Institutional Relations & Congress Manager
Excellence Director N.B. Should one of the above attendees be identified in the case report, they will be excluded from any decision related to that caseNeumann Anne-Katrin
Czech Republic
Belgium
Spain
Poland
UK
Southeast Europe
Ireland
Turkey
Netherlands
Sarah Dodd (UK)
Associate Director, Employee Communications
PA to General Manager
Format fulfil its Bily Kuo (EMEA) The committee willLene Freij (Nordic & Baltic Operations) Communications Manager, responsibilities via email
EMEA
Switzerland
Carol Hammond (EMEA)
Greece
Russia & CIS
Nordic & Baltic Operations
France
Italy
Portugal
MENA/SSA
Germany
Corporate Communications
Project Manager, Communication & Commercial Excellence
Alex Orton (EMEA)
Kathrin Garcia (Switzerland)
Communications Officer
Field Market Access Manager
Jo Taylor (EMEA)
Beatrice Huber (Germany)
Senior Director, Corporate Communications
PA to Director Marketing
Emma White (EMEA)
Giota Korovesi (Greece)
Communications Manager
Executive Assistant & Communications Coordinator
Margot Kubosch (Spain) Corporate Affairs & Communications Manager
CLIENT
PROJECT
WORK TYPE
Astellas
Print and digital marketing material
• New Business Visualisations • E-Marketing Designs • Website Design • Infographics
(Switzerland)
Senior Manager Market Access
Frequency Karinaby Oppitz (Germany) On a case case basis Manager Communications
Catarina Silva (E6 - Portugal) HR Manager
Eliska Strosova (Czech Republic) HR Associate
Simona Sutaviciute (MENA/SSA) Regional Communications, PR and Events Manager
Tatiana Vanderstraeten (Belguim) PA to General Manager
Azra Pisek (South East Europe)
Yda Visser (The Netherlands)
Office Manager & PA
Management & Communication Coordinator
Barbara te Riele (The Netherlands)
Karen Welby (Ireland)
Manager Communications
Lee Roberts (E6 - Hub) HR Director
Executive Assistant
Elzbieta Wrzesinska (Poland) PA to GM / Assistant in E&C Dept.
Justine Foucault Serre (France) Business Intelligence & Services Team Manager, Marketing Corporate Communication Manager, General Management
Esra Yazici (Turkey)
CLIENT
Astellas OVERACTIVE BLADDER (OAB)
AFFECTS AROUND
Living with Prostate Cancer
OVERACTIVE
ADULTS IN THE UK
The Every Voice Matters survey provides an in-depth analysis and personal insight into the lives of 141 UK men with prostate cancer.1 The UK survey results have been taken
AFFECTS AROUND
7 MILLION 1
ONE THREE
OVER
OVER
50%
URGENCY a sudden, compelling desire to pass urine
OAB
which is difficult to defer1. This symptom is also regarded as a driver for other symptoms:
URINARY INCONTINENCE OR ‘WET’ OAB – any involuntary leakage of urine
5
FREQUENCY– the need to empty the bladder more
8x
than eight times in a day5
NOCTURIA
– awakening at night one or more times to empty the bladder5
When asked what matters most since being diagnosed with prostate cancer...
THE EMBARASSING SITUATIONS LEAGUE TABLE6
83% WETTING YOURSELF IN PUBLIC
1%
red wine on someone else’s white carpet
TESTING?
4%
1%
the wrong person
ONE THREE
Nearly in women don’t feel comfortable talking about it with their GP2
IS MORE COMMON
than arthritis3, angina4 and diabetes2
SYMPTOMS OF
SPILLING
7 MILLION
WHAT MATTERS MOST
OAB
of people diagnosed with OAB don’t feel comfortable talking about their waterworks with friends or family2
6%
BLADDER (OAB) ADULTS IN THE UK1
The survey was commissioned by Astellas.
Nearly in don’t feel comfortable talking about it with their GP2
50%
from a pan-European survey of 668 men diagnosed with prostate cancer, designed to determine unmet needs in the current care and management of patients.1
FALLING over in public
Being
OVERHEARD
having a private conversation
TELLING
1%
a joke no one laughs at
?
19%
10%
men highlighted the importance of living well2
spending time with family and friends2
OAB
of women diagnosed with OAB don’t feel comfortable talking about their waterworks with friends or family2
IS MORE COMMON
than arthritis3, angina4 and diabetes5
URGENCY a sudden, compelling desire to pass urine
SYMPTOMS OF
OAB
12%
17% enjoying life2
of men said that being cured is what matters most2
which is difficult to defer6,7. This symptom is also regarded as a driver for other symptoms:
URINARY INCONTINENCE OR ‘WET’ OAB6 – any involuntary leakage of urine FREQUENCY6– the need to empty the bladder
8x
more than eight times in a day
NOCTURIA8– awakening at night more than twice
QUALITY OF LIFE MATTERS Quality of life is very important to men diagnosed with prostate cancer
to empty the bladder
THE EMBARASSING SITUATIONS LEAGUE TABLE9
1 in 5 (20%) men feel quality of life is more important than living longer3
Being
1%
3 in 4 (74%) men feel a good quality of life is as important as being able to live longer with treatment3
compared to only 1 in 17 (6%) who feel living longer is more important3
CONTRIBUTING TO SOCIETY IS IMPORTANT
50% 40% 30% 20%
MEN
Having to get up to
A partner snoring
Noise from other
A partner fidgeting
MEN
Needing to get a
red wine on someone else’s white carpet
FALLING
over in public
?
TELLING
a joke no one laughs at
1%
TEXTING
1%
BEING OVERHEARD
the wrong person
having a private conversation
VS
BEING STOOD UP on a date
WOMEN10
WHAT ANNOYS US MOST AT NIGHT TIME
continue to contribute to society
0%
yourself in public
1%
It is important for men to remain well enough to
10%
SPILLING
1%
VS ALL CHARTS ARE REF 6
WETTING
6% 4%
STOOD UP on a Date
80%
WOMEN
50% 40% 30%
30% 20% 10% 0%
20% 10%
Wetting yourself in a
Being shown up at
Dating mishaps
Parents Grandparents showing bad
The majority of patients (87%) said they want to fight their cancer, and 2 in 5 (41%) want to continue working as much as possible4,5
UK men are working for longer – there are currently
0%
A partner snoring
Having to get up to use the toilet
>600,000 men in the UK
Needing to get a drink of water
Noise from other rooms/flats
A partner fidgeting
over the retirement age, but still working6
N W
MEN
E S
MEN
THE ROLE OF HEALTHCARE PROFESSIONALS
66%
68%
Men feel that
65% 61%
continuity of care is important when making treatment choices
50%
Just over half of women and two fifths of men believe lifestyle advice to be the standard treatment for people with Overactive Bladder. Two fifths of men and a third of women believe that medicine is standard treatment
30% Surgery
Patients with prostate cancer also feel that they communicate
well with their doctor
10% 0%
Wetting yourself in a public place
Being shown up at school
Dating mishaps
Parents showing bad baby photos
Just over half of women and two fifths of men believe lifestyle advice to be the standard treatment for people with OAB. Two fifths of men and a third of women believe that medicine is standard treatment
Lifestyle advice (modify liquid intake/bladder/training)
agree it is important to see the same consultant over the course of their treatment7
77%
say they are well informed about their disease9
Medicine
30%
52%
42%
Grandparents/ parents
OAB TREATMENT11
40%
42%
WOMEN
20%
Surgery
Medicine
WOMEN10
30%
50%
95% Lifestyle advice (modify liquid intake/bladder)
VS
WHAT WE FOUND MOST EMBARRASSING AS KIDS
66%
There were very slight regional variations in awareness of OAB with respondents living in the North, South West and East showing the highest levels and those in London and the South East showing the lowest levels.
40%
42%
52%
42%
10% 11%
Nothing, it’s an inevitable part of ageing
10% 11%
83%
Nothing, it’s an inevitable part of
7% 7%
agree that their nurse plays an important role in answering their questions8
62%
feel they are able to influence their treatment choice with their healthcare professional10
References: 1. Abrams P et al. Reviewing the ICS 2002 Terminology Report: The Ongoing Debate. Neurourol Urodyn 2006; 25:293-294 2. Joint Health Surveys Unit (2006) Health Survery for England 2006. Prevalence of diagnosed diabetes by sex and age. The Information Centre: Leeds 3. Reginster JY. The prevalence and burden of arthritis. Rheumatology 2002; 41(Suppl 1):3-6 4. Joint Health Surveys Unit (2008) Health Survey for England 2006. Cardiovascular disease and risk factors. The Information Centre: Leeds 5. Abrams P et al. The standardisation of terminology of lower urinary tract function: Report from the standardisation sub-committee of the international continence society. Neurourol Urodyn 2002; 21:167-178 6. ICM Research, Overactive Bladder Research, October 2012
7% 7% References: 1. Astellas Pharma Ltd. Data on File. STAR Number 363714 – January 2012 2. Astellas Pharma Ltd. Data on File. STAR Number 392706 – October 2012 3. Reginster JY. Rheumatology 2002; 41(Suppl 1):3-6. 4. Joint Health Surveys Unit (2008) Health Survey for England 2006. The Information Centre: Leeds. 5. Joint Health Surveys Unit (2006) Health Survery for England 2006. Prevalence of diagnosed diabetes by sex and age. The Information Centre: Leeds 6. Abrams P et al. The standardisation of terminology of lower urinary tract function: Report from the standardisation sub-committee of the international continence society. Neurourol Urodyn 2002; 21: 167-178. 7. Abrams P et al. Reviewing the ICS 2002 Terminology Report: The Ongoing Debate. Neurourol Urodyn 2006; 25: 293-294 8. Milsom I. et al. How widespread are the symptoms of an overactive bladder and how are they managed? A population-based prevalence study. BJU International 2001; 87(9): 760-766 9. Astellas Pharma Ltd. Data on File. STAR Number 397996 – January 2013 10. Astellas Pharma Ltd, Data on File, VES13037UKa February 2013 11. Astellas Pharma Ltd, Data on File, VES13037UK February 2013
visit bladderproblem.co.uk for further information This is part of an awareness campaign sponsored by Astellas Pharma Ltd. Date of preparation: April 2013 Job number: VES12485UKe(1)
OF THE 141 MEN SURVEYED FROM THE UK: 16%
CLIENT
PROJECT
Astellas Oncology
Print and digital marketing material
had localised prostate cancer – cancer that is only in the prostate gland and has not spread to another part of the body 11,12
WORK TYPE
10%
3%
had metastatic castration-resistant prostate cancer (mCRPC) – cancer that may have become resistant to medical or surgical treatments 11,14
49%
had locally advanced disease – cancer that is high risk of growing or spreading within a few years 11,12
were in remission – when tests, physical exams, and scans show that all signs of your cancer are gone 11,15
had advanced/metastatic prostate cancer – cancer that has spread beyond the prostate (or metastasized) into to the lymph nodes or other parts of the body 11,13
The remaining sample did not know the stage of their disease
• New Business Visualisations 14% • E-Marketing Designs • Website Design • Infographics
14%
Some respondents provided more than one answer about their current diagnosis.
1.
Astellas. Every Voice Matters UK survey results. Data on File - Sample size XTD15232UK 2. Astellas. Every Voice Matters UK survey results. Data on File – What matters most XTD15234UK 3. Astellas. Every Voice Matters UK survey results. Data on File – Quality of life XTD15235UK 4. Astellas. Every Voice Matters UK survey results. Data on File - Plan to fight the cancer XTD15236UK 5. Astellas. Every Voice Matters UK survey results. Data on File - Continue to work as much as possible XTD15237UK 6. Department for Work and Pensions, Older People’s Day: 1 million in work over 65: 3 years since end of default retirement age. Available at: https://www.gov.uk/government/news/older-peoples-day-1-million-in-work-over65-3-years-sinceend-of-default-retirement-age. [Last accessed January 2016] 7. Astellas. Every Voice Matters UK survey results. Data on File - Continuity of care XTD15238UK 8. Astellas. Every Voice Matters UK survey results. Data on File - Importance of nurse XTD15239UK
Date of preparation: February 2016 Job number: XTD15199UK
9. Astellas. Every Voice Matters UK survey results. Data on file - Well informed about the disease XTD15240UK 10. Astellas. Every Voice Matters UK survey results. Data on File - Influence on treatment choice XTD15241UK 11. Astellas. Every Voice Matters UK survey results. Data on File – Stage of PCa XTD15233UK 12. Cancer Research UK, Risk factors in localised prostate cancer. Available at: http://www.cancerresearchuk.org/about-cancer/type/prostate-cancer/treatment/ types/risk-factors-in-localised-prostate-cancer. [Last accessed January 2016] 13. WebMD, Prostate Cancer Health Center. Available at:http://www.webmd.com/ prostate-cancer/tc/prostate-cancer-advanced-ormetastatic-topic-overview. [Last accessed January 2016] 14. Cancer.Net, Treatment of Metastatic Castration-Resistant Prostate Cancer. Available at: http://www.cancer.net/research-and-advocacy/asco-careandtreatment-recommendations-patients/treatment-metastatic-castrationresistantprostate-cancer. [Last accessed January 2016] 15. WebMD, Remission: What does it mean? Available at: http://www.webmd.com/ cancer/remission-what-does-it-mean. [Last accessed January 2016]
eed any sk your
CLIENT
AstraZeneca Continue to use your Duaklir® Genuair® in just a few simple steps:
The colour of your Duaklir® Genuair® inhaler has changed from a white and turquoise cap and dosage button to white with an orange cap and dosage button.
INFORMATION FOR PATIENTS
1
Your inhaler has changed colour
Remove cap before use
2
Hold with the orange button facing straight up. DO NOT TILT
3
PRESS the orange button all the way down
ATTENTION: DO NOT HOLD THE ORANGE BUTTON DOWN WHILE YOU ARE INHALING
GREEN
4
RELEASE the orange button
The medicine that is taken from the inhaler has not been changed and you should continue to use the inhaler as shown previously by your doctor, nurse or pharmacist.
5
Ready to use
6
CORRECT
RED
INCORRECT
7
Inhaled correctly
8
Replace cap after use
ADVERTISEMENT FEATURE
Joint Working Project Objective
Step 4: Working with secondary care
• Reduce unwarranted variation and deliver consistent standards of care across the entire pathway for patients with asthma from the CCG’s 18 practices
• Data sharing between the hospital trust and practices was established to allow proactive case management by practices following A&E attendance
Joint Working Project Strategy
• Standardisation of hospital paperwork was agreed and that a discharge summary would be sent by the hospital to a patient’s practice to allow primary care follow up within 7 days
IWork together with NHS Improvement, practices, patients, PCT pharmacists, the Local Prescribing Committee (LPC) and secondary care specialists to create centralised guidance, education and resources that allow practices to autonomously manage their asthma patients in the most effective and efficient manner.
Working Together in Practice Step 1: Consistent patient cohorting
AstraZeneca Joint Working Case Study Improving Asthma Care in Partnership with NHS East Surrey CCG
• AstraZeneca provided a data interrogation tool which defined specific cohorts to help practices group and manage their patients — Four cohorts were identified and profiled - with the largest being patients who were receiving asthma medications but had not received a formal diagnosis – which went on to inform the types of other resources required • Risk stratification was a key outcome, and through three “Plan Do Study Act” cycles, four key cohorts were identified through risk stratification for intervention Step 2: Creating central resources
Executive Summary Following a successful Joint Working project focusing on COPD, NHS East Surrey CCG approached NHS Improvement to participate as an asthma test site for the Lung Improvement Programme. This gave the CCG an opportunity to improve asthma patient care, and reduce unnecessary spending by optimising and standardising the approach taken to the condition’s management across their 18 practices. Through a second Joint Working project with AstraZeneca, and in collaboration with local stakeholders, the CCG was able to develop a fully integrated pathway that focused on every aspect from case finding and accurate diagnosis, chronic disease management, through to acute care. This allowed practices to: • a 21% reduction in COPD hospital bed days • reduce emergency asthma hospital admissions by 21%i, and • increase patient recognition of having a formal self-management plan up to 73%i The success of the project was recognised across the NHS when it was nominated as a finalist at the 2012 National Association of Primary Care (NAPC) Vision Awards.
• From the cohort profiling, the team developed standardised read codes and two types of formal self-management plans – one pictorial and one text-based – for use by practices with patients • Local asthma diagnostic guidelines and a treatment pathway were developed in line with the BTS/SIGN Guideline, in a collaboration between the medicines management team, PCT pharmacists, LPC representatives and patients from each practice Step 3: Engaging and upskilling practices • An asthma education day was held with guest speaker, Professor Martyn Partridge, which was attended by 60 GPs and nurses • Practice specific cohort breakdowns were presented individually to practices alongside the management resources to enable and empower them to put in plan appropriate plans of action • AstraZeneca nurses helped mentor practice nurses on optimal management for different cohorts • PCT pharmacists visited practices to carry out medication reviews and went into care homes to do patient medication reviews • A monthly newsletter was developed by the project team to keep all practices up to date on project progress
AstraZeneca and Joint Working
Situation
Improving patient lives is at the heart of AstraZeneca’s business. In the UK the primary customer for our medicines, and consequent partner in helping us achieving that goal, is the NHS.
Following a highly successful COPD focused Joint Working project that NHS East Surrey CCG and AstraZeneca worked on together, the partnership embraced the opportunity to take on a new challenge to tackle the variation in asthma care across the CCG’s 18 practices.
The ambitions of the NHS are broad and wide ranging, and it faces many challenges in achieving all it wants for people across the UK. As a result, NHS organisations are increasingly calling on external expertise to help them to meet these challenges. This ‘Joint Working’ approach is one that is actively promoted by key industry bodies including the Department of Health and the ABPI (Association of the British Pharmaceutical Industry). AstraZeneca is committed to Joint Working as a means of supporting the NHS to achieve more for patients, and welcomes the opportunity to pool skills, experience and/or resources for the joint development and implementation of patient centred projects and share a commitment to successful delivery.
Key Outcomes Primary successes: • Willing and engaged practices across the CCG, allowing the new tools and guidelines to become the natural way of consulting, and standardised optimal care becoming the norm • BTS step recording went from 4% to 20%
AstraZeneca Joint Working Pulling together for patient care – highlighting the success of Joint Working initiatives
• Compliance recording increased by 7%iv • Recording of inhaler technique increased by 813 patients iv • 454 extra patients had a self-management planiv • Within the identified high risk group, improvement from 24.6% to 73.1% who were aware of having a self-management plani • 58 additional patients were referred for smoking cessationiv ‘Some increase in prescribing costs did occur, but as a consequence of the prevalence of people with asthma increasing through correct diagnosis and treatment, as well as some initial medication wastage due to therapy adjustments.’ Lizzette Howers, Primary Care Pharmacist, NHS Surrey ‘The project has been a real success for the 18 practices across the CCG and has clearly demonstrated that case finding, standardised management and medicines optimisation improves asthma care for patients, joins up the efforts of healthcare professionals working with asthma patients across the healthcare spectrum and has the potential to result in important cost savings for the NHS.’ Dr Elango Vijaykumar Respiratory Lead, East Surrey CCG ‘We have now worked on a number of successful Joint Working projects with AstraZeneca and the outcomes have been extremely valuable to the CCG. More importantly however they have had a real impact for patients and healthcare professionals in the East Surrey community. The amount that we can achieve when we pull together, pooling resources and expertise, is really impressive and proves we can do things better together.’ Dr Joe McGilligan, Chair of East Surrey CCG and Co-Chair Surrey Health and Wellbeing Board
Executive Summary A recent series of Joint Working initiatives across the country has resulted in reductions in hospital admissions, significant cost savings and empowered patients. These outcomes result from a number of Joint Working partnerships between AstraZeneca and NHS organisations around the UK, focused on working together to deliver excellence in patient-centred care. In its drive to fulfil its commitment to improving patients’ lives, and in line with the Department of Health’s definition of Joint Working, AstraZeneca has partnered with the NHS to achieve more for patients by pooling skills, experiences and resources for the joint development and implementation of patient-centred projects. The following examples below highlight the significant benefits of a successful, collaborative approach to patient care.
OneHeart
STAIRS (Stockport Airways Project)
AstraZeneca and the Bristol Heart Institute (BHI) are currently working together to improve treatment adherence in patients with acute coronary syndrome (ACS), by introducing the OneHeart programme – a personalised patient support service that addresses unhelpful beliefs that can lead to a patient’s non-adherence to prescribed medical treatment through a range of tailored interventions.
Stockport CCG, formerly Stockport Managed Care, identified that there was scope for improvement in their area’s management of Chronic Obstructive Pulmonary Disease (COPD). AstraZeneca and Stockport CCG collaborated to develop a steering group (STAIRS) which placed trained respiratory nurses within 12 practices with the highest rates of COPD-related hospital admissions to assess and improve patient identification of those most at risk and review in line with NICE guidance. These skills were then evaluated in all Stockport CCG-based Practice Nurses, and further training was offered.
Anecdotal feedback from the team at BHI suggests that they have already seen some early success in terms of better patient understanding of their illness and proactivity in seeking further information. “Our collaboration with AstraZeneca, through the OneHeart project, has already demonstrated the positive impact of NHS and Industry partnerships for patients.” Dr Tom Johnson, Consultant at Bristol Heart Institute The OneHeart programme will continue until 2016, with the ultimate aim of reducing re-admissions to hospital.
The prevalence of asthma in England is amongst the highest in the world, estimated to affect 3 to 5.4 million people . Between 1,000 -1,200 people a year still die from asthma in England, and it is estimated that 90% of those deaths are attributed to preventable factorsii. Asthma is managed predominately in primary care with patients taking responsibility for lots of the management of their condition themselves outside of the healthcare setting. Despite emergency admission rates being low (84 in 2010/11 ) across the CCG’s patient population, it was recognised that the care patients received from the 18 practices was variable and that this variation could lead to suboptimal patient outcomes and ultimately unnecessary spending.
Caption to film
Caption to film
This targeted activity resulted in: • Between December 2008 – June 2010 there was a 40% reduction in highrisk COPD patients’ hospital admissions (vs. 7% reduction in the remaining Stockport CCG practices)1 • £70,500 cost savings as a result of the reduced hospital admissions, which could result in a total saving of £210,000 if applied across the group2 “I believe Joint Working with the right partner not only brings fantastic benefits to patients and potential cost savings to the NHS, but enhances the day to day working practices of our NHS teams.” Dr Jaweeda Idoo, Clinical Director of Services Transformation, Stockport CCG
To read more about the successes of the Joint Working initiatives that AstraZeneca has successfully implemented in partnership with the NHS, please visit http://www.astrazeneca.co.uk/astrazeneca-in-uk/who-dowe-work-with/working-with-the-nhs. To discuss a potential Joint Working initiative with us, please contact Jack Wood, Head of Field Medical Operations on 01582 836000, or your local AZ Regional Account Manager.
References 1. Pulse Practical Commissioning, Raising the Asthma Care Bar, Dr Vijaykumar, December 2012. 2. Department of Health, An outcomes strategy for people with chronic obstructive pulmonary disease (COPD) and asthma in England, 18 July 2011. Accessed on 14.12.2012 via http://www.dh.gov.uk/en/Publicationsandstatistics/Publications/PublicationsPolicyAndGuidance/DH_127974 3. South East Coast Quality Observatory , EsyDoc hospital admissions with asthma as a primary diagnosis (18 + yrs), 2012 4. NHS Improvement – Lung, Improving adult asthma care: Testing the case for change, August 2012
AZ respiratory offerings and partnerships are endorsed by the NAPC
References
12 | Section or brochure name
Section or brochure name | 13
1. Stockport Airways Project Overview, 2012 2. AstraZeneca Data on File (DOF SYM\113\May2012)
Date of Preparation: September 2013 Atlas ID: 2702503
There is also a drive nationally and locally to minimise prescribing costs. The priority areas locally are respiratory and gastro. Dermatology is not a priority area, as the overall spend on dermatology prescribing is relatively low. This is confirmed by the local health economy websites.
BILL
+ +
ALWAYS CONSCIOUS OF TREATMENT COSTS.
BOB I know from Dr Maria and the practice team that many patients with psoriasis are struggling to control their condition. Genalcitrol is usually the first line for mild to moderate psoriasis.
POST-CALL ACTIONS AUTHORITY LEVEL This is a fictional scenario and fictional medications. These materials are intended for selling skills training and development purposes only. Proprietary and Confidential AZ document – For internal training use only. © 2018 AstraZeneca All local training/communication should be signed off via the applicable MC process Approval ID: Z4-8464 Date of Preparation: 08/12/2017 Expiry date: 08/12/2019
CLIENT
PROJECT
WORK TYPE
AstraZeneca
Print and digital marketing material
• • •
Editorial Layouts New Business Visualisations Website Design
After that, the patient pathway moves to topical steroids, alone or in combination with genalcitrol. Stronger steroids may be prescribed if needed.
Then patients are frequently referred to the specialists – who may well prescribe vitamin D analogues and steroids, before using systemic treatments and UV therapy. And several patients will require management for co-morbidities such as anxiety or even depression.
CLIENT
Bayer KNOWING WHERE TO GO FOR SUPPORT AND MORE INFORMATION FOR YOURSELF AND YOUR LOVED ONE There are many sources of information, especially on the internet, including chat forums and blogs etc. Additionally there are patient support telephone helplines and groups.* It’s important to make sure that the information you are accessing is reliable and accurate. Healthcare professionals are best placed to provide you with reliable advice and to direct you to reliable sources of information. Patient.info patient.info/health/prostate-cancer-leaflet
Patient Support Groups Many patients and their families and loved ones find attending a support group really helps them. People often imagine support groups to consist of sitting in a circle and one by one telling the group about themselves and their experiences. This isn’t the case. They more commonly involve talks and activities not limited to prostate cancer, besides offering information and disease-management advice from professionals and patients who have had a similar experience. Most importantly, attending a group is a chance to meet other people going through a similar experience. Don’t underestimate the positive impact this face-to-face contact can have.
The Manversation campaign has been developed in consultation with leading prostate cancer charities, Orchid — Fighting Male Cancer and Tackle Prostate Cancer. The campaign has been organised and funded by Bayer.
THINGS TO CONSIDER WHEN A LOVED ONE HAS BEEN GIVEN A DIAGNOSIS OF PROSTATE CANCER
Orchid - Fighting Male Cancer orchid-cancer.org.uk Helpline: 0808 802 0010 Tackle Prostate Cancer tackleprostate.org
The Patient.info website provides comprehensive health information, including information about the diagnosis, assessment and management of prostate cancer.
HELPING YOU HAVE A CONVERSATION ABOUT PROSTATE CANCER
To find your nearest support group, speak to your healthcare team who will be able to advise you. You can also access information via patient organisations.
Support group location finder: tackleprostate.org/find-asupport-group-near-you.php Helpline: 0800 035 5302 Manversation manversation.co.uk
When you find out that a loved one has prostate cancer it can be as scary for you as it is for him. You are likely to have a lot of questions and to want to try to support your loved one as best you can. Through this journey there are likely to be times when you need to have difficult conversations, from speaking to your loved one to speaking to the doctors and nurses and telling other family members and friends.
The Manversation website provides more information including a similar guide for your loved one with prostate cancer. The Manversation campaign has been developed in consultation with leading prostate cancer charities Orchid - Fighting Male Cancer and Tackle Prostate Cancer. The campaign has been organised and funded by Bayer.
* Bayer does not take responsibility for the content of materials provided from the listed organisations.
More than a third of diabetic patients will develop some level of macular oedema1
Follow our live updates on
7th March 2019 #OphthHonours
1. Macular Society. Your guide to diabetic macular oedema. Available at: https://www. macularsociety.org/sites/default/files/resource/Accessible%20MS025%20DMO%20 FEB17pdf .pdf (Last accessed: October 2020)
October 2020 | XXXXXXXXXXX
Sponsored by
Prostate Cancer In the UK, prostate cancer is the most common cancer in men and the 2nd most common cause of cancer-related death in men1
48k+
men in the UK are diagnosed with prostate cancer every year, on average.1 Despite having hormone therapy, a proportion of these patients will have disease progression to castration-resistant prostate cancer (CRPC)2
About
There are several unmet needs that need to be addressed4,5
3
of men with non-metastatic castration-resistant prostate cancer (nmCRPC) go on to develop metastases within two years2
Unmet Need In Prostate Cancer Prostate cancer treatments have advanced in recent years, but unmet needs persist4,5
1
6
%
of men upon their diagnosis of prostate cancer present with cancer that has spread from the original (primary) tumour3
Overall Survival
It is vital for patients across all stages of prostate cancer to have treatment options that may help to improve their overall survival6
Role of Side Effects Delay Progression
Ophthalmology Honours
EYLEA® (aflibercept) now available in pre-filled syringe
2018/19 The Uveitis Service Building a holistic personalised service for patients with sightthreatening inflammation University Hospitals Birmingham NHS Foundation Trust
Treatments for prostate cancer may have challenging side effects which can impact quality of life8
Progression to metastasis increases the risk of mortality and morbidity, reduces quality of life and increases healthcare costs7
Honouree Best Ophthalmology Team
Prostate Cancer References 1. Cancer Research UK. Prostate Cancer Statistics. https://www.cancerresearchuk.org/health-professional/cancer-statistics/statistics-by-cancer-type/prostate-cancer? Accessed October 2020. 2. Kirby M. et al. Characterising the castration-resistant prostate cancer population:a systematic review. Int J Clin Pract. 2011;65(11):1180-1192. doi:10.1111/j.1742-1241.2011.02799. 3. Terris M. Metastatic and Advanced Prostate Cancer: Overview, Epidemiology of Advanced Prostate Cancer, Presentation of Advanced Prostate Cancer. Medscape. https://emedicine.medscape.com/article/454114-overview. Published 2018. Accessed October 2020. 4. Hussain, M., Fizazi, K., Saad, F. et al. Enzalutamide in men with nonmetastatic, castration-resistant prostate cancer. N Engl J Med. 2018;378:2465–2474. 5. Smith, M.R., Saad, F., Chowdhury, S. et al. Apalutamide treatment and metastasis-free survival in prostate cancer. N Engl J Med. 2018;378:1408–1418. 6. Fizazi K, Shore N, Tammela T, et al. Darolutamide In Nonmetastatic Castration-Resistant Prostate Cancer. N Engl J Med. 2019;380(7). 7. Hong J, Kim IY et al. Nonmetastatic Castration-Resistant Prostate Cancer. Korean J Urol. 2014;55(3):153. doi:10.4111/kju.2014.55.3.153. 8. Tannock et al. Docetaxel plus Prednisone or Mitoxantrone plus Prednisone for Advanced Prostate Cancer. N Engl J Med. 2004;351:1502-12. doi:10.1056/NEJMoa040720. © 2020 Bayer plc. All rights reserved. BAYER and the Bayer Cross are registered trademarks of Bayer.
Ophthalmology Honours is an educational initiative fully funded by Bayer. The judging process is carried out by a panel of independent judges and is wholly independent of Bayer.
The recently launched EYLEA® (aflibercept) pre-filled syringe (PFS) is now available in the UK across all NHS Trusts, providing an alternative method of intravitrial injection for physicians.
Bayer is working closely with centres to provide support where possible, including investigating innovative solutions such as the community-based macular service established in Manchester.3
The EYLEA PFS requires fewer steps to prepare than the standard glass vial, giving physicians a choice of option that works best for them, their patients and the efficiency of their clinic.
Over 1.5 million people in the UK have macular disease, over a third of these have wet AMD with nearly 40,000 new cases arising every year.4,5
ABOUT EYLEA Tight binding affinity EYLEA has a higher binding affinity for VEGF-A than native receptors, ranibizumab or bevacizumab, in vitro6†
EYLEA is indicated for adults for the treatment of neovascular (wet) age-related macular degeneration (AMD), visual impairment due to macular oedema secondary to retinal vein occlusion (branch RVO or central RVO), visual impairment due to diabetic macular oedema (DMO) and visual impairment due to myopic choroidal neovascularisation (myopic CNV).1
DURABLE
Multi-target MOA EYLEA is the only anti-angiogenic agent licensed for intraocular use that binds to VEGF-B, PiGF and galectin-1,‡ in addition to all known VEGF-A isoforms1,6,8-11
PATIENT CARE DURING THE COVID-19 CRISIS The Royal College of Ophthalmologists’ guidance of 30 March provides a pragmatic approach to care during the COVID-19 pandemic. The guidance outlines maintenance of care for those who need it, while deferring care for those patients who can wait.2
EYLEA has an established safety profile,1 with over 30 million doses administered worldwide since launch12
Deferral of existing patient clinical review for 4 months (with exceptions) has been advised for patients with DMO, branch RVO or central RVO.2
GLOSSARY: Fc: Fragment crystallisable IgG1: Immunoglobulin G1 MOA: Mode of action PiGF: Placental growth factor VEGF-A: Vascular endothelial growth factor A VEGF-B: Vascular endothelial growth factor B
All patients already under hospital review for wet AMD should maintain an 8-weekly dosing regimen of anti-VEGF therapy with no clinical review unless they mention a significant drop in vision at their injection visit.2 EYLEA offers the option to treat wet AMD patients proactively with either a fixed 8-weekly dosing regimen, or a treat-and-extend regimen with up to 16-week intervals.1
PP-EYL-GB-0596 | May 2020
Durable EYLEA includes the Fc portion of a human IgG1 antibody, which provides stability and durable anti-VEGF activity7-9
Prescribing information can be found on the next page † Bevacizumab is not licensed for intraocular use6 Data obtained in vitro6
‡
Eylea® 40 mg/ml solution for injection in a vial & Eylea® 40 mg/ml solution for injection in pre-filled syringe (aflibercept) Prescribing Information (Refer to full Summary of Product Characteristics (SmPC) before prescribing) Presentation: 1 ml solution for injection contains 40 mg aflibercept. Vial: Each vial contains 100 microlitres, equivalent to 4 mg aflibercept. Pre-filled syringe (PFS): Each PFS contains 90 microlitres, equivalent to 3.6 mg aflibercept. Indication(s): Treatment of neovascular (wet) age- related macular degeneration (wAMD), macular oedema secondary to retinal vein occlusion (branch RVO or central RVO), visual impairment due to diabetic macular oedema (DMO) in adults and visual impairment due to myopic choroidal neovascularisation (myopic CNV). Posology & method of administration: For intravitreal injection only. Must be administered according to medical standards and applicable guidelines by a qualified physician experienced in administering intravitreal injections. Each vial or PFS should only be used for the treatment of a single eye. Extraction of multiple doses from a single vial or PFS may increase the risk of contamination and subsequent infection. The vial or PFS contains more than the recommended dose of 2 mg. The extractable volume of the vial (100 microlitres) or PFS (90 microlitres) is not to be used in total. The excess volume should be expelled before injecting. Refer to SmPC for full details. Adults: The recommended dose is 2 mg aflibercept, equivalent to 50 microlitres. For wAMD treatment is initiated with 1 injection per month for 3 consecutive doses. The treatment interval is then extended to 2 months. Based on the physician’s judgement of visual and/or anatomic outcomes, the treatment interval may be maintained at 2 months or further extended using a treat-andextend dosing regimen, where injection intervals are increased in 2- or 4-weekly increments to maintain stable visual and/or anatomic outcomes. If visual and/or anatomic outcomes deteriorate, the treatment interval should be shortened accordingly to a minimum of 2 months during the first 12 months of treatment. There is no requirement for monitoring between injections. Based on the physician’s judgement the schedule of monitoring visits may be more frequent than the injection visits. Treatment intervals greater than 4 months between injections have not been studied. For RVO (branch RVO or central RVO), after the initial injection, treatment is given monthly at intervals not shorter than 1 month. Discontinue if visual and anatomic outcomes indicate that the patient is not benefiting from continued treatment. Treat monthly until maximum visual acuity and/or no signs of disease activity. Three or more consecutive, monthly injections may be needed. Treatment may then be continued with a treat-andextend regimen with gradually increased treatment intervals to maintain stable visual and/or anatomic outcomes, however there are insufficient data to conclude on the length of these intervals. Shorten treatment intervals if visual and/or anatomic outcomes deteriorate. The monitoring and treatment schedule should be determined by the treating physician based on the individual patient’s response. For DMO, initiate treatment with 1 injection/month for 5 consecutive doses, followed by 1 injection every 2 months. No requirement for monitoring between injections. After the first 12 months of treatment, and based on visual and/or anatomic outcomes, the treatment interval may be extended such as with a treat-and-extend dosing regimen, where the treatment intervals are gradually increased to maintain stable visual and/or anatomic outcomes; however there are insufficient data to conclude on the length of these intervals. If visual and/or anatomic outcomes deteriorate, the treatment interval should be shortened accordingly. The schedule for monitoring should therefore be determined by the treating physician and may be more frequent than the schedule of injections. If visual and anatomic outcomes indicate that the patient is not benefiting from continued treatment, treatment should be discontinued. For myopic CNV, a single injection is to be administered. Additional doses may be administered if visual and/or anatomic outcomes indicate that the disease persists. Recurrences should be treated as a new manifestation of the disease. The schedule for monitoring should be determined by the treating physician. The interval between 2 doses should not be shorter than 1 month. Hepatic and/or renal impairment: No specific studies have been conducted. Available data do not suggest a need for a dose adjustment. Elderly population: No special considerations are needed. Limited experience in those with DMO over 75 years old. Paediatric population: No data available. Contraindications: Hypersensitivity to active substance or any excipient; active or suspected ocular or periocular infection; active severe intraocular inflammation. Warnings & precautions: As with other intravitreal therapies endophthalmitis, intraocular inflammation, rhegmatogenous retinal detachment, retinal tear and iatrogenic traumatic cataract have been reported. Aseptic injection technique is essential. Patients should be monitored during the week following the injection to permit early treatment if an infection occurs. Patients must report any symptoms of endophthalmitis or any of the above mentioned events without delay. Increases in intraocular pressure have been seen within 60 minutes of intravitreal injection; special precaution is needed in patients with poorly controlled glaucoma (do not inject while the intraocular pressure is ≥30 mmHg). Immediately after injection, monitor intraocular pressure and perfusion of optic nerve head and manage appropriately. There is a potential for immunogenicity as with other therapeutic proteins; patients should report any signs or symptoms of intraocular inflammation e.g pain, photophobia or redness, which may be a clinical sign of hypersensitivity. Systemic adverse
PP-EYL-GB-0596 | May 2020
PP-PF-OPHT-GB-0009-1 | January 2019
PROJECT
WORK TYPE
Bayer
Manversation - BOH marketing materials
• Editorial Layouts • Social Media Content • Gifs • E-Marketing Designs
Eylea® is a trademark of the Bayer Group Adverse events should be reported. Reporting forms and information can be found at www.mhra.gov.uk/yellowcard or search for MHRA Yellow Card in the Google Play or Apple App Store. Adverse events should also be reported to Bayer plc. Tel.: 0118 2063500, Fax.: 0118 2063703, Email: pvuk@bayer.com © Bayer plc. ® Registered trademark of BAYER AG, Germany.
1. Bayer 2019. Eylea 40mg/ml solution for injection SmPC. Available at https://www.ema.europa.eu/en/documents/product-information/eylea-epar-product-information_en.pdf. Accessed May 2020 2. RCOphth 2020. Medical Retinal Management Plans during COVID-19. Available at https://www.rcophth.ac.uk/wp-content/uploads/2020/03/Medical-Retinal-Management-Plan-during-COVID-19-UPDATED-300320-1-3. pdf. Accessed May 2020 3. Bayer 2018. New services launched in Manchester bring vital eye care to the high street. Available at https://www.bayer.co.uk/en/media/latest-news/new-services-launched-inmanchester-bring-vital-eye-care-to-the-high-street.php. Accessed May 2020 4. Macular Society 2018. Nearly 1.5m people in the UK are affected by macular disease. Available at https://www.macularsociety. org/news/nearly-15m-people-uk-are-affected-macular-disease. Accessed May 2020 5. NICE 2018. Age-related macular degeneration. Available from https://www.nice.org.uk/guidance/ng82/chapter/ Context. Accessed May 2020 6. Papadopoulos N, et al Binding and neutralization of vascular endothelial growth factor (VEGF) and related ligands by VEGF Trap, ranibizumab and bevacizumab. Angiogenesis 2012;15:171-185 7. Regeneron Pharmaceuticals Inc Traps. Available at https://www.regeneron.com/technology. Accessed May 2020 8. EMA. EYLEA EPAR assessment report 2012. Available at https:// www.ema.europa.eu/en/documents/assessment-report/eylea-epar-public-assessment-report_en.pdf. Accessed May 2020 9. Rudge JS, et al. VEGF Trap complex formation measures production rates of VEGF, providing a biomarker for predicting efficacious angiogenic blockade. Proc Natl Acad Sci USA 2007;104:18363-18370 10. Kanda A, et al. Aflibercept Traps Galectin-1, an Angiogenic Factor Associated with Diabetic Retinopathy. Sci Rep 2015;5:17946 11. Amadio M, et al. Targeting VEGF in eye neovascularization: What’s new?: A comprehensive review on current therapies and oligonucleotide-based interventions under development. Pharmacol Res 2016;103:253-269 12. Data on file 2019. Ref EYLO010_30 million vials of EYLEA sold worldwide
PP-UN-ONC-GB-0043 | October 2020
CLIENT
events including non-ocular haemorrhages and arterial thromboembolic events have been reported following intravitreal injection of vascular endothelial growth factor (VEGF) inhibitors. Safety and efficacy of concurrent use in both eyes have not been systemically studied. No data is available on concomitant use of Eylea with other anti-VEGF medicinal products (systemic or ocular). Caution in patients with risk factors for development of retinal pigment epithelial tears including large and/or high pigment epithelial retinal detachment. Withhold treatment in patients with: rhegmatogenous retinal detachment or stage 3 or 4 macular holes; with retinal break and do not resume treatment until the break is adequately repaired. Withhold treatment and do not resume before next scheduled treatment if there is: decrease in best-corrected visual acuity of ≥30 letters compared with the last assessment; central foveal subretinal haemorrhage, or haemorrhage ≥50%, of total lesion area. Do not treat in the 28 days prior to or following performed or planned intraocular surgery. Eylea should not be used in pregnancy unless the potential benefit outweighs the potential risk to the foetus. Women of childbearing potential have to use effective contraception during treatment and for at least 3 months after the last intravitreal injection. In patients presenting with clinical signs of irreversible ischaemic visual function loss, aflibercept treatment is not recommended. Populations with limited data: There is limited experience in DMO due to type I diabetes or in diabetic patients with an HbA1c over 12% or with proliferative diabetic retinopathy. Eylea has not been studied in patients with active systemic infections, concurrent eye conditions such as retinal detachment or macular hole, or in diabetic patients with uncontrolled hypertension. This lack of information should be considered when treating such patients. In myopic CNV there is no experience with Eylea in the treatment of non-Asian patients, patients who have previously undergone treatment for myopic CNV, and patients with extrafoveal lesions. Interactions: No available data. Fertility, pregnancy & lactation: Not recommended during pregnancy unless potential benefit outweighs potential risk to the foetus. No data available in pregnant women. Studies in animals have shown embryo- foetal toxicity. Women of childbearing potential have to use effective contraception during treatment and for at least 3 months after the last injection. Not recommended during breastfeeding. Excretion in human milk: unknown. Male and female fertility impairment seen in animal studies with high systemic exposure not expected after ocular administration with very low systemic exposure. Effects on ability to drive and use machines: Possible temporary visual disturbances. Patients should not drive or use machines if vision inadequate. Undesirable effects: Very common: Visual acuity reduced, conjunctival haemorrhage (wAMD phase III studies: increased incidence in patients receiving anti-thrombotic agents), eye pain. Common: retinal pigment epithelial tear (known to be associated with wAMD; observed in wAMD studies only), detachment of the retinal pigment epithelium, retinal degeneration, vitreous haemorrhage, cataract (nuclear or subcapsular), corneal abrasion or erosion, increased intraocular pressure, blurred vision, vitreous floaters, vitreous detachment, injection site pain, foreign body sensation in eyes, increased lacrimation, eyelid oedema, injection site haemorrhage, punctate keratitis, conjunctival or ocular hyperaemia. Serious: cf. CI/W&P - in addition: blindness, culture positive and culture negative endophthalmitis, cataract traumatic, transient increased intraocular pressure, vitreous detachment, retinal detachment or tear, hypersensitivity (during the post-marketing period, reports of hypersensitivity included rash, pruritus, urticaria, and isolated cases of severe anaphylactic/anaphylactoid reactions), vitreous haemorrhage, cortical cataract, lenticular opacities, corneal epithelium defect/erosion, vitritis, uveitis, iritis, iridocyclitis, anterior chamber flare, arterial thromboembolic events (ATEs) are adverse events potentially related to systemic VEGF inhibition. There is a theoretical risk of arterial thromboembolic events, including stroke and myocardial infarction, following intravitreal use of VEGF inhibitors. As with all therapeutic proteins, there is a potential for immunogenicity. Consult the SmPC in relation to other side effects. Overdose: Monitor intraocular pressure and treat if required. Incompatibilities: Do not mix with other medicinal products. Special Precautions for Storage: Store in a refrigerator (2°C to 8°C). Do not freeze. Unopened vials and unopened syringe blisters may be stored at room temperature (below 25°C) for up to 24 hours before use. Legal Category: POM. Package Quantities & Basic NHS Costs: Single vial or PFS pack: £816.00 MA Number(s): EU/1/12/797/001-002. Further information available from: Bayer plc, 400 South Oak Way, Reading RG2 6AD, United Kingdom. Telephone: 0118 206 3000. Date of preparation: April 2020.
• PowerPoint Presentations • Website Design • Infographics
CHOLESTEROL AWARENESS 29% of over 45s
Almost 45% of over 45s have no idea what their cholesterol level is
CLIENT
Benecol
have never had a cholesterol test,
25%
8% said they weren’t currently doing anything about their cholesterol level
8%
WHO IS YOUR PLUS-ONE
DID YOU KNOW…? A daily intake of 1.5 –2.4g plant stanols is proven to lower LDL cholesterol by 7 – 10% in 2 to 3 weeks
VS
19%
34% of women
said they were more worried about their partner’s cholesterol than their own
Cholesterol affects 3 out of 5 adults in the UK1
72%
In contrast,
of men
only 19%
said they were more worried about their partner’s cholesterol than their own
FOODS AND ACTIVITIES THAT HELP TO REDUCE CHOLESTEROL
But in fact,
raised cholesterol affects
men and women over 45 equally2
One in four of those aged 45 and over already take between 3 and 6 prescription meds every day
Eating cholesterol lowering functional foods that contain plant stanols or plant sterols is clinically proven to lower LDL cholesterol
HEALTH AND WELLBEING
94
2nd
%
of people over 45 years old say maintaining their heart health is “extremely important” to them
39% 39
%
Heart disease ranks second among this groups health concerns
Eating more fruits and vegetables 72% say they would prefer to lower their cholesterol through diet and exercise alone
72%
are worried about cholesterol which is a major risk factor in the development of heart disease
But 25% of people are unaware that (functional) foods and drinks containing Plant Stanols are proven to lower cholesterol
Reducing dairy products Reducing red meats Eating more wholegrains & oats
25%
Eating more fish Eating more soya
CHOLESTEROL AWARENESS Almost 45% of over 45s have no idea what their cholesterol level is
Exercise
29% of over 45s
have never had a cholesterol test,
45
* Based on research undertaken by Redshift Research on behalf of Benecol amongst
DID YOU KNOW…?
2000 people over 45 in the UK
A daily intake of 1.5 –2.4g plant stanols is proven to lower LDL cholesterol by 7 – 10% in 2 to 3 weeks
rising to 40% in the 45 to 54 year old population
%
But 25% of people are unaware that (functional) foods and drinks containing Plant Stanols are proven to lower cholesterol
rising to 40% in the 45 to 54 year old population
45%
Cholesterol By Numbers*
72% say they would prefer to lower their cholesterol through diet and exercise alone
References: 1. Heart UK, ‘Cholesterol – The Silent Killer http://heartuk.org.uk/files/uploads/documents/HUK_memberapplicationform.pdf (Accessed 25th February 2014) 2. Townsend N, Wickramasinghe K, Bhatnagar P, Smolina K, Nichols M, Leal J, Luengo-Fernandez R, Rayner M (2012). Coronary heart disease statistics 2012 edition. British Heart Foundation: London.
May 2014
8% said they weren’t currently doing anything about their cholesterol level
8%
!
AIM YOUR PLUS-ONE WHO IS Collect 5 different fruit foam
% 34 5 A DAY
FOODS AND ACTIVITIES THAT HELP TO REDUCE CHOLESTEROL
VS
Eating cholesterol lowering functional foods that contain plant stanols or plant sterols is clinically proven to lower LDL cholesterol
pieces along the assault course. Once all 5 pieces are collected they get to throw them into a giant cup with the message ‘one % of your 5 a day’. Each piece of fruit will have a fact about it.
19
of women said they
In contrast,
of men
were more worried about their partner’s cholesterol than their own
only 19%
said they were more worried about their partner’s cholesterol than their own
ORANGES Oranges contain vitamin C and folate. I'll look after your immune system and help reduce tiredness
Eating more fruits and vegetables But in fact,
Reducing dairy products
raised cholesterol affects
men and women over 45 equally2
Reducing red meats
BANANAS I'm a good source of potassium for normal blood pressure, muscle function and the nervous system One in four of those aged 45 and over
Eating more wholegrains & oats
already take between 3 and 6 prescription meds every day
Eating more fish Eating more soya
72% say they would prefer to lower their cholesterol through diet and exercise alone
72%
But 25% of people are unaware that (functional) foods and drinks containing Plant Stanols are proven to lower cholesterol PINEAPPLE I'm a good source of vitamin C, which helps % immune system your
25
RASPBERRY
Exercise I'm a source of
manganese which helps keep bones APPLE Based on research undertaken healthyby Redshift Research on behalf of Benecol amongst I'm a *good source 2000 people over 45 in the UK of vitamin C to A DAY support your immune system References:
5
1. Heart UK, ‘Cholesterol – The Silent Killer http://heartuk.org.uk/files/uploads/documents/HUK_memberapplicationform.pdf (Accessed 25th February 2014) 2. Townsend N, Wickramasinghe K, Bhatnagar P, Smolina K, Nichols M, Leal J, Luengo-Fernandez R, Rayner M (2012). Coronary heart disease statistics 2012 edition. British Heart Foundation: London.
May 2014
CLIENT Benecol
DID YOU KNOW…? PROJECT A daily intake ofMarketing 1.5 –2.4gmaterial plant stanols is proven to lower LDL cholesterol by 7 – 10% in 2 to 3 weeks
FOODS AND ACTIVITIES THAT HELP TO REDUCE CHOLESTEROL
WORK TYPE
• Editorial Layouts • Social Media Content • New Business Visualisations • Infographics
SHOOT THE FRUIT Once all the fruit pieces are collected the participants can then throw into the fruit bin.
CLIENT
Gilead Everyone with hepatitis C is entitled to receiving care. Hep C is treatable and curable in the majority of patients.
Ambassador Newsletter ISSUE 1 | OCTOBER 2017
Hep C affects thousands of people in the UK. You might be among those living with the day-to-day reality of being infected with a virus that can cause permanent damage to the liver, and potential health problems in other parts of the body.
It is important to remember that hep C is a virus; it is not something that defines you as a person. You’re worth the best care and treatment. The longer you have lived with hep C, the more likely it is that your liver may be damaged and your health in the long-term could be affected. If you have hep C, don’t ignore it; speak to your doctor to find out what treatment and care options are right for you.
• Presentations by I’m Worth… ambassadors Louise and Brian at meetings in Wales and to support World Hepatitis Day in July • The addition of new ambassadors to support the campaign and further its reach across the UK • A survey in Drink and Drug News to identify community needs through those working in addiction services
Visit
Information for people living with hep C
World Hepatitis Day 2017 Thank you for your continued support to the I’m Worth… campaign! It’s been an exciting few months for the campaign; some highlights include:
www.imworth.co.uk
In this first edition of your campaign newsletter, you can read more about the recent campaign activities and find out how you can get more involved in the coming months!
for more information, useful resources and to hear about others experiences
We know a number of you were able to attend the Hepatitis C Trust’s patient conference in London on World Hepatitis Day (28th July) and were able to hear from advocates and community members from around the world affected by hepatitis C. We spoke to Brian, who said;
“This day is an opportunity to reduce the stigma by educating people. It’s still a relatively unknown disease to many people, even those that are most at risks from it” You can read more about Brian’s experience during World Hepatitis Day on the I’m Worth… website here: www.imworth.co.uk/ world-hepatitis-daymatters-view-imworth-ambassadorbrian
Did you or your community do anything to mark World Hepatitis Day? If so, we’d love to hear about your experience and what World Hepatitis Day means to you.
Stock imagery, posed by models July 2017 | HCV/UK/16-04/CI/1422b
July 2017 | HCV/UK/16-04/CI/1422b
By 2030 Approximately 3 in 4 people with HIV in Europe will be over 501 HIV
THE
LONG VIEW
Developed and funded by
References: 1. Vance DE et al. Predictions of geriatric HIV in 2030. Lancet Infect Dis. 2015;15(7):753–754 2. Guaraldi G et al. Aging with HIV vs. HIV Seroconversion at Older Age: A Diverse Population with Distinct Comorbidity Profiles. PLoS One. 2015;10(4):e0118531 UNBC4086 | December 2016
CLIENT
PROJECT
WORK TYPE
Gilead
‘I’m Worth’ marketing material
• Editorial Layouts • Social Media Content • Gifs • E-Marketing Designs
• PowerPoint Presentations • Website Design • Infographics
October 2017 | HCV/UK/17-04/NM/1558j
CLIENT
ViiV Healthcare Kivexa®: Confidence from the start
Kivexa: Confidence from the start A trusted foundation: Well-known tolerability and efficacy profile
A trusted foundation: Well-known tolerability and efficacy profile
Simplicity: A single HLA-B*5701 test and low additional product-specific monitoring
Simplicity and flexibility: · A single HLA-B*5701 test
Flexibility: Once-a-day dosing, with or without food, and few drug-drug interactions
· Low additional productspecific monitoring · Once-a-day dosing with or without food · Few drug interactions · Suitable for use with a variety of 3rd agents
In treatment-naïve patients
RAPID RESPONSE AND STATISTICALLY SUPERIOR EFFICACY VS DRV/r UP TO 96 WEEKS1,2*
EFFECTIVE REGARDLESS OF BASELINE VIRAL LOAD1,2
FLAMINGO—Proportion of treatment-naïve patients with HIV-1 RNA <50 copies/mL up to 96 weeks (N=484)1,2
FLAMINGO—Proportion of treatment-naïve patients with HIV-1 RNA <50 copies/mL at 48 and 96 weeks in high viral load subgroup (n=122)1,2
Proportion (%) of patients HIV-1 RNA <50 copies/mL
90
New 96-week data from the
FLAMINGO Study
TIVICAY IS SUPERIOR TO DRV/r UP TO 96 WEEKS IN TREATMENT-NAÏVE PATIENTS WITH HIV1,2
80
83%
70 60
68%
50 40 30 20
P =0.025
10
Presented at the HIV Drug Therapy Glasgow Meeting 2-6 November 2014
80%
Week
0
4
8
12 16
24
36
48
P =0.002 60
72
84
Darunavir/r 800 mg/100 mg QD + 2 NRTIs (n=242)
on therapy.
Adapted from Clotet et al, 2014.1,2
Statistically superior virological response at 48 and 96 weeks
1,2
More rapid virological response with TIVICAY vs DRV/r—87% vs 31%, respectively, at Week 82 Virological response was higher for TIVICAY vs DRV/r, regardless of NRTI backbone1
Group of Companies nc code: UK/DLG/0055/13(4)
A HIGH BARRIER TO RESISTANCE UP TO 96 WEEKS1,2
ng forms and information and, adverse events should vigilance Section, Health n 2, Tel: +353 1 676 4971, ported to GlaxoSmithKline 5 in Ireland.
0% treatment-emergent resistance in either arm
93%
82%
90
70%
80 70
52%
60 50 40 30 20 10 57/61
96
Weeks 48 and 96 snapshot analyses.
TIVICAY 50 mg QD + 2 NRTIs (n=242)
100
Proportion (%) of patients HIV-1 RNA <50 copies/mL
90%
100
43/61
50/61
Week 482 Baseline viral load
32/61
Week 961 >100,000 copies/mL
TIVICAY 50 mg QD + 2 NRTIs
Darunavir/r 800 mg/100 mg QD + 2 NRTIs Adapted from Clotet et al, 2014.1,2
In patients with baseline viral load >100,000 copies/mL, greater virological response at Weeks 48 and 96 with TIVICAY vs DRV/r1,2
GENERALLY WELL TOLERATED UP TO 96 WEEKS1,2 Diarrhoea was more common in patients receiving DRV/r (24% vs 10%) Significantly fewer patients receiving TIVICAY had ≥Grade 2 fasting LDL values vs DRV/r (3% vs 10%; P<0.001)
*From an open-label, multicentre study comparing TIVICAY 50 mg once daily plus abacavir/lamivudine or tenofovir/emtricitabine or DRV/r 800 mg/100 mg once daily plus abacavir/lamivudine or tenofovir/emtricitabine.2
HIV Drug Therapy Glasgow et al. Lancet. 2014;383:2222cteristics.
er 2014. VIIV/DLG/0116/14a
f ficacy
Prescribing Information can be found on the back cover.
Beyond Ef ficacy
Prescribing Information can be found on the back cover.
CLIENT
PROJECT
WORK TYPE
Kivexa Tivicay
Isell detail aid and marketing materials
• • •
Editorial Layouts New Business Visualisations PowerPoint Presentations
Beyond Ef ficacy
CLIENT
ViiV Healthcare 17.10.2013
A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: August 2013. Job Code: VIIV/HIV/0038/13
17.10.2013
Square Brussels | Gold Hall | Thursday 17th October 2013 | 18.15-19.45
Square Brussels | Gold Hall | Thursday 17th October 2013 | 18.15-19.45 Take part in a different kind of symposium chaired by Professor Brian Gazzard Join experts in HIV and patient centred care to investigate the development of an HIV decision-aid in real time.
Just another
HIV
THINK
AGAIN
symposium?
AGENDA Prof. Brian Gazzard , UK
Beyond the evidence base My HIV. My Life. A personal perspective
Video
The importance of being involved
Sandra Van den Eynde, Belgium
Are we prepared to manage HIV as a chronic condition?
Prof. Andrew Miles, UK
Collaborative care in action: creating a decision aid in real time
Panel discussion facilitated by Prof. Andrew Miles
Meeting summary and close
Prof. Brian Gazzard, UK
Panel members: Prof. Brian Gazzard, UK Sandra Van den Eynde, Belgium Prof. Jürgen Rockstroh, Germany Prof. Gilles Pialoux, France
THINK AGAIN
Just another HIV symposium?
Take part in a different kind of symposium chaired by Professor Brian Gazzard Join experts in HIV and patient centred care to investigate the development of an HIV decision-aid in real time.
Speakers and panelists: Professor Brian Gazzard, Sandra Van den Eynde, Professor Andrew Miles Professor Gilles Pialoux Professor Jürgen Rockstroh
AGENDA
Just another HIV symposium?
Beyond the evidence base
Prof. Brian Gazzard , UK
My HIV. My Life. A personal perspective
Video
The importance of being involved
Sandra Van den Eynde, Belgium
Are we prepared to manage HIV as a chronic condition?
Prof. Andrew Miles, UK
Collaborative care in action: creating a decision aid in real time
Panel discussion facilitated by Prof. Andrew Miles
Meeting summary and close
Prof. Brian Gazzard, UK
Panel members: Prof. Brian Gazzard, UK Sandra Van den Eynde, Belgium Prof. Jürgen Rockstroh, Germany Prof. Gilles Pialoux, France
THINK AGAIN A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: September 2013. Job Code: BE/HIV/0025/13 Not for distribution
Lectern Panel
17.10.2013
703mm
Lectern Panel with Screen
450mm
Square Brussels | Gold Hall | Thursday 17th October 2013 | 18.15-19.45
1920 pixels
Just another HIV symposium?
Just another HIV symposium?
THINK AGAIN Take part in a different kind of symposium chaired by Professor Brian Gazzard Join experts in HIV and patient centred care to investigate the development of an HIV decision-aid in real time.
Just another HIV symposium?
THINK AGAIN
THINK AGAIN
THINK AGAIN
1163mm
1080 pixels
1100mm
Speakers and panelists: Professor Brian Gazzard, Sandra Van den Eynde, Professor Andrew Miles Professor Gilles Pialoux Professor Jürgen Rockstroh
FRONT VIEW
A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: September 2013. Job Code: BE/HIV/0017/13
A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: September 2013. Job Code: BE/HIV/0015/13
Not for distribution
SIDE VIEW
FRONT VIEW
Not for distribution
Just another HIV symposium?
THINK AGAIN A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: September 2013. Job Code: BE/HIV/0020/13
A Satellite Symposium organised and funded by ViiV Healthcare ©2013 ViiV Healthcare group of companies All rights reserved. Date of preparation: September 2013. Job Code: BE/HIV/0020/13
Not for distribution
Not for distribution
CLIENT
PROJECT
WORK TYPE
ViiV Healthcare
HIV Symposium
• Conference Materials • Editorial Layouts • PowerPoint Presentations
CLIENT
ViiV Healthcare
AGENDA
M E N U
Wednesday 24th October AUDIENCE All All
Crossfunctional group split Crossgroup split
LIGHTHOUSE MEETING:
DOLUTEGRAVIR LOC ACTIVATION MEETING DATES:
Monday 22nd (Evening), 2012 Tuesday 23rd, 2012 Wednesday 24th October, 2012
VENUE:
Millbank Tower, 21-24 Millbank Westminster, London, SWIP 4QP
All
TIME
SESSION OUTLINE
PRESENTER(S)/ FACILITATOR LEAD(S)
AUDIENCE
08.30 – 08.45
Opening speech – Day Two
Michael Grant Gregory Reinaud
All
08.45 – 09.15
Tactical Launch Plan Plenary
Tom Williams Jon Greggs Nathalie Dang
All
09.15 – 12.15
Tactical Launch Plans Interactive Workshop Session
Katie Lipscombe & team CrossCross-functional facilitators functional group split
12.15 – 12.45
Working Lunch Break
12.45 – 13.30 functional
Lighthouse Identity
13.30 – 14.00
Building a Local DTG Launch Plan – Launch Excellence Framework and Key Deliverables Plenary
Saskia Fontein
Observation Deck 3 Workshop
Crossgroup split
Ulrike Mucha Jason Coull Sara LeClerc Dustin Haines
STARTER Beetroot-marinated and grilled Claire Island organic salmon hand-picked white crab, crunchy shaved fennel, white anchovies and dill salad
LIGHTHOUSE MEETING:
DOLUTEGRAVIR LOC ACTIVATION MEETING
Question for the team?
MAIN
Dry-aged fillet of Cumbrian beef with wild mushroom crust, roasted winter vegetables and fondant potato
DATES:
All VENUE:
Monday 22nd (Evening), 2012 Tuesday 23rd, 2012 DESSERT Wednesday 24th October, 2012 Trio of vanilla seed creme brulee Millbank Tower, 21-24 Millbank single origin chocolate and Westminster, London, SWIP 4QP
To:
Question:
zesty lemon curd tart
Vegetarian option available on request
AGENDA
AGENDA
Monday 22nd October
Monday 22nd October
TIME
SESSION OUTLINE
PRESENTER(S)/ FACILITATOR LEAD(S)
AUDIENCE
TIME
SESSION OUTLINE
PRESENTER(S)/ FACILITATOR LEAD(S)
AUDIENCE
19.00 – 21.30
Welcome Reception Welcome Speech with hot buffet at Millbank Tower
Tom Laughery Jonathan Anderson
All
19.00 – 21.30
Welcome Reception Welcome Speech with hot buffet at Millbank Tower
Tom Laughery Jonathan Anderson
All
LIGHTHOUSE MEETING :
DOLUTEGRAVIR LOC ACTIVATION
DIRECTIONS
Millbank Tower 21 - 24 Millbank London, SW1P 4QP
Double Tree Hotel
22 - 24 October 2012 | Millbank Tower | London
From:
Maurizio Amato ITALY
From Double Tree Hotel Double Tree Hilton Hotel Westminster, London, SW1P 4DD Approximately 4 minutes by foot Directions on Foot Turn right on John Islip St towards Page St Turn right onto Page Street Turn right onto Thorney Street Turn right onto Millbank Slight right to stay on Millbank Destination on the right Millbank Tower
CLIENT
PROJECT
WORK TYPE
ViiV Healthcare
Dolutegravir Symposium
• Conference Materials • PowerPoint Presentations
CLIENT
LEO Pharma LEO Pharma UK/IE presents
LEO Pharma UK/IE presents
D E R M ATA L K
DERM CONNEXT 27th November 2020
Inaugural Virtual Event.
INAUGURAL VIRTUAL EVENT
VIEW DETAILS
27th November 2020 Agenda and Speakers
— we help people achieve healthy skin
— we help people achieve healthy skin
DERM CONNEXT
NEWS
OCTOBER 2020 | SUBJECT: MOSAIC NEWS
Session Agenda
Dear all, We wanted to take this opportunity to thank you for attending the 2020 MOSAIC virtual launch event. The 2-day meeting was a milestone for the MOSAIC project, which we hope you found both enjoyable and enlightening.
We are keen to collate as many thoughts and feedback on MOSAIC as possible so we can use this to shape the program moving forward. If you haven’t done so already, please click on the below link to complete the evaluation form. Thank you in advance for your honest response:
people to look under the skin of psoriasis to see the seriousness treatment options and improved access to care for the 125 million people who are living with the condition today.
treatment options and improved access to care for the 125 million people who are living with the condition today.
Often regarded as ‘just a skin condition’; psoriasis is in fact a serious, lifelong disease that carries with it a number of potentially life-limiting comorbidities. ‘I’m more than my skin’ aims to increase understanding of psoriatic disease and its comorbidities.
a serious, lifelong disease that carries with it a number of
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potentially life-limiting comorbidities. ‘I’m more than my skin’ aims to increase understanding of psoriatic disease and its comorbidities.
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Evaluation form
‘I’m More Than My Skin’, an awareness campaign. By asking of the disease, the campaign aims to advocate for better
Often regarded as ‘just a skin condition’; psoriasis is in fact
Copy 2
World Psoriasis Day 2018 sees the launch of LEO Pharma’s
‘I’m More Than My Skin’, an awareness campaign. By asking of the disease, the campaign aims to advocate for better
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I’m more than my skin
World Psoriasis Day 2018 sees the launch of LEO Pharma’s people to look under the skin of psoriasis to see the seriousness
Copy 1
Feedback
I’m more than my skin
For more information about the campaign, visit
www.immorethanmyskin.com
For more information about the campaign, visit
www.immorethanmyskin.com
Copy 4
https://mosaic2020.com/attendee/#ss--MGNaYbe00KgXdmp5acy
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Meeting summary From tackling the clinical challenges associated with psoriasis to getting your first real look at the MOSAIC app we hope you found the virtual launch training valuable and thought-provoking.
Models are for illustrative purposes only.
Models are for illustrative purposes only.
Thank you for engaging in such fruitful, constructive and open exchanges throughout the presentations and workshops. Special thanks to the steering committee presenters Professor Peter van de Kerkhof, Dr Anna López-Ferrer and Dr Athanasios Tsianakas for their role in delivering high quality educational content and invaluable insights into the value of MOSAIC.
Let’s keep in touch — MOSAIC teams channel We have taken the opportunity to create a MOSAIC teams channel to keep in touch and share thoughts as we lead up to the official MOSAIC app rollout in 2021. Please do join the group to keep the conversation going; you will have received a link from Kasper Vadstrup. We encourage you to reach out with any feedback or questions in relation to MOSAIC. We hope the virtual MOSAIC launch event has left you feeling energized and excited for introducing MOSAIC into your HCP engagements and benefiting from more insightful interactions.
What’s coming next? From now until the launch we will be providing you with lots of different resources to help utilize MOSAIC once available, including: • Virtual Coffee and Connect sessions • e-learning modules • Case study and MOSAIC handbooks
More information will follow but do keep a lookout in our newsletters to keep up to date.
As always, if you have any questions feel free to get in touch. Kasper Vadstrup Senior Global Scientific Advisor Global BioDermatology +45 3137 5114 VPDDK@leo-pharma.com
Majid Sheikh Medical Science Liaison LEO Pharma UK/IE +447825919184 mshuk@leo-pharma.com
CLIENT
PROJECT
WORK TYPE
Leo Pharma
Various marketing materials
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
• E-Marketing Designs • PowerPoint Presentations • Infographics
CLIENT
LEO Pharma
Psoriasis is a common and complex disease
Brodalumab
tions Communica it Launch Toolk
Social stigma places a heavy burden and can negatively impact mental health1
14 million in Europe
Affects
125million
have experienced 77% stigmatisation
3
1
people worldwide2
BEGIN
Two to three-fold risk of anxiety and depression 2
Many types Job Code: XXXXX | Date of Preparation: October 2017
97%
Plaque psoriasis
of patients1
is most common affecting up to
COMMUNICATIONS TOOLKIT
In a study
INTRODUCTION
Severity DEAR COLLEAGUE
~25
How to use the Kyntheum® Communications Launch Toolkit
Welcome to the Kyntheum® Communications Launch Toolkit. The launch of Kyntheum® represents a significant milestone for LEO Pharma. For the first time ever, we will be able to offer people living with psoriasis a biologic treatment. This will enable us to help more people overcome their skin disease and live positive lives.
Patient Advocacy Group (PAG) Engagement Plan
The guidance within this Toolkit has been developed to support markets to prepare for and engage with the media and other important stakeholders to support the launch of Kyntheum®. The aim is to support you in delivering an effective and engaging launch which is suited for your market.
Sourcing case studies/ambassadors
Prior to any use, please ensure that all activities are compliant with local regulations before implementation. All the materials will require local adaptation and approval. The Global Communications Team would love to assist you and see the results of your good work. Please do share your questions, learnings and successes with us so that we can learn from your experiences and pass them on to other colleagues.
Cost
Social media
Feelings of
or
anger
helplessness
44%
for patients and healthcare systems
Marie Schleimann Nordlund Senior Global Patient Communication Manager Bio Dermatology, Global Commercial Strategy marie.nordlund@leo-pharma.com
often or always depressed because
among psoriasis patients also translate into higher rates of suicidal ideation compared to other patients1
Significant costs
On behalf of the Bio Dermatology team, good luck with your media launch!
of people
of psoriasis3
will have moderate-tosevere psoriasis4
Sourcing spokespeople
Media outreach
46%
with moderate-to-severe psoriasis reported being
References 1. World Health Organization (WHO). Global Report on Psoriasis. 2016; 2. The International Federation of Psoriasis Associations. Home page; 3.Ortonne J 2004; 4. Mantovani L et al. Dermatol Ther. 2016 Jun; 6(2):151-167
increased risk
of suicidal ideation and behaviour compared to the general population4
References 1. World Health Organization (WHO). Global Report on Psoriasis. 2016; 2. Dalgard F, et al. JID. 2015;135(4), 984-991; 3. Weiss SC, et al. J Am Acad Dermatol. 2002;47:512-18; 4. Kurd et al, Arch Dermatol 2010;146(8):891-895
2
People with moderate-tosevere psoriasis have a two to three-fold risk of anxiety and depression 4
SYMPTOMS
• Brodalumab delivered almost clear skin (PASI 90) or completely clear skin (PASI 100) in more than three-quarters (76.8%, n= 779) and more than half (56.2%, n=779) of patients after 120 weeks of treatment, respectively
This meeting will provide an interactive forum in which we will discuss and seek input on our planned patient activities and campaigns.
• The proportions of patients achieving high levels of skin clearance were comparable at year one (week 52) and year two (with 78% and 53% of patients achieving PASI 90 and PASI 100, in year one respectively)
Ahead of the advisory board meeting we will share pre-read materials and an agenda to help you prepare for the meeting.
If you haven’t done so already, please contact me at morgane.cuisenier@leo-pharma.com in regards to flight and accommodation booking. We very much look forward to welcoming you to Copenhagen. Best wishes,
Static Physician Global Assessment (sPGA)
Psoriasis Area and Severity Index (PASI)
• Clinical assessment tool that ranges from mild to very severe and is a physician’s overall impression of the severity of the psoriasis at a single point [BAD, psoriasis worksheet]
• Used in clinical trials to indicate a % change in disease; i.e. PASI 75 = 75% reduction in disease severity. PASI 90 or 100 indicates almost clear or completely clear skinand personal relationships compared with placebo
Morgane Cuisenier Global Public Affairs Associate LEO Pharma A/S
People with psoriasis have a
44 % increased risk of suicidal ideation and behaviour compared to the general population 5
DIAGNOSIS
• At week 120, brodalumab continued to be well-tolerated with a comparable safety profile as observed in the 52-week studies
We will also contact you to enter into a written agreement about your participation in the advisory board.
Most frequently reported symptoms are scaling and thickening of the skin, itching and erythema (reddening of the skin) 3
IMPACTS
There are several types of psoriasis, of which plaque psoriasis is the most common affecting up to
RESULTS • 1604 patients entered the long term extension (140 mg Q2W, n=158; 210 mg Q2W, n=1392; 140 mg Q4W, n=40; 140 mg Q8W, n=14); total exposure was 3228.5 years
The efficacy and safety of Kyntheum® was evaluated in three clinical trials: AMAGINE-1 comparing Kyntheum® to placebo and AMAGINE-2 and -3 comparing Kyntheum® to placebo and ustekinumab 5
In a study
Psoriasis can vary from moderate to severe and the systemic (entire body) nature often remains unrecognised*
46 % of people with moderate-to-severe psoriasis reported being often
or always depressed because of psoriasis 6
* Other comorbid diseases, such as metabolic syndrome, chronic obstructive pulmonary disease, asthma, peptic ulcer disease, liver disease, renal failure, and rheumatoid arthritis, have also been associated with a diagnosis of psoriasis7 1 2 3
4 5 6 7
April 2017
THREE STUDIES
th
As a global patient centric company with the vision of becoming the preferred dermatology care partner, LEO Pharma very much welcomes the input of our key stakeholders to help us develop and shape our advocacy activities and ensure that they benefit patients, first and foremost. The advisory board meeting is being held to gather valuable insights and opinions from a number of patient organisations across different countries. We would very much appreciate your input based upon your professional experience and expertise in the area of psoriasis, specifically, supporting people with the condition.
Kyntheum® (brodalumab) is a self-injectable IL-17 biologic for the treatment of moderateto-severe psoriasis5 that can give a high level of skin clearance 6 and sustained response for patients who are candidates for systemic treatment3
with psoriasis say that they have experienced stigmatisation 1
97 % of patients3
Date: 8 June 12.00 to 9 June 13.00 (CET) Location: Norstat Frederiksborggade 1, 1360, Denmark th
Achieving rapid 1,2 and sustained 3 complete skin clearance4 (or PASI 100, where PASI refers to the Psoriasis Area Severity Index, and 100 denotes free from visible disease) is a desirable treatment outcome
A NEW TREATMENT
Assessment (sPGA) score of 0 (clear) and/or 1 (almost clear); PASI 75/90/100; exposure-adjusted incidence of adverse events switched to brodalumab 210mg Q2W. At week 52 ustekinumab patients switched to brodalumab 210mg Q2W.
Thank you for your interest and confirming your attendance at the LEO Pharma Global Patient Organisations Advisory Board Meeting – details below:
Psoriasis is associated with social stigma, which can negatively impact mental health 3
77 % of people TYPES
Key endpoints evaluated at week 120: static Physician Global
Dear invitee,
About Kyntheum®
(brodalumab)
Psoriasis is a common, chronic, immune-mediated inflammatory disease that primarily involves the skin
Trial design: patients were randomized 2:2:1:1 to brodalumab 140 or 210mg every 2 weeks (Q2W), ustekinumab or placebo, respectively. At week 12, brodalumab patients were re-randomized (2:2:2:1) to 140 or 210mg Q2W, 140mg Q4W or 140mg Q8W; placebo patients switched to brodalumab 210mg Q2W.
Factsheet for journalists
The International Federation of Psoriasis Associations. Available at: https://ifpa-pso.com/ (Accessed July 2017) Ortonne J, et al. Eur J Dermatol. 2004;14:41–45 World Health Organization (WHO). Global Report on Psoriasis. Available from: http://apps.who.int/iris/bitstr am/10665/204417/1/9789241565189_eng.pdf (Accessed July 2017) Dalgard F, et al. JID. 2015;135(4), 984-991 Kurd et al, Arch Dermatol 2010;146(8):891-895 Weiss SC, et al. J Am Acad Dermatol. 2002;47:512-18 Yeung H, et al. JAMA Dermatol. 2013;149(10):1173-1179
Job Code: XXXXX | Date of Preparation: August 2017
CLIENT
PROJECT
WORK TYPE
Leo Pharma
Various marketing materials
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
• E-Marketing Designs • PowerPoint Presentations • Infographics
The trials in total 5 included 4,373 patients with moderate-to-severe psoriasis, the largest study population in the development program of any new biologic treatment in psoriasis to date6,7,8,9,10,11
At week 2 1 in 4 patients reached PASI 75 after two weeks of treatment in clinical trials 12
FINDINGS
About Psoriasis
Dr Mark Lebwohl et al. P1790
8-9th June, Copenhagen
worldwide live with psoriasis1
14,000,000 in Europe2
UNMET NEED
Brodalumab provides robust and sustained levels of efficacy in moderate-to-severe psoriasis: 120 weeks of treatment in the AMAGINE 2 study.
LEO Pharma Global Patient Organisations Advisory Board Meeting
125 million people
Approximately twice as many patients on Kyntheum® achieved complete clearance (PASI 100) compared to patients treated with ustekinumab in the AMAGINE-2 (44 % versus 22 %) and AMAGINE-3 (37 % versus 19 %) studies 4
7 in 10 patients reported psoriasis no longer impaired their health-related quality of life compared with placebo 3
At week 52 More than half of patients (53-56%) maintained complete clearance of their psoriasis (PASI 100) and three quarters (75%) achieved almost clear skin (PASI 90) 3
When almost clear or completely clear of psoriasis symptoms (PASI 90 / 100), people experience greater improvements in their health-related quality of life than patients with a lower treatment response13 With current available treatments, many patients achieve only incomplete clearance, and treatment discontinuation rates are high.14 Kyntheum® offers patients the opportunity to achieve high levels of skin clearance3 and improved health-related quality of life15
Data from the three large randomised, controlled AMAGINE clinical trials, found Kyntheum® to be well tolerated, with an acceptable safety profile.16,17 The most common adverse events were arthralgia (joint pain), nasopharyngitis (inflammation of the nose and pharynx), headache, and upper respiratory tract infection 4 1. Russell CB, et al. J Immunol. 2014; 192: 3828-36 2. Papp K, et al. The American Academy of Dermatology annual meeting 2017. Poster 4978 3. Supplement to: Lebwohl M, et al. N Engl J Med 2015;373:1318-28 4. Lebwohl M, et al. N Engl J Med 2015;373:1318-28 5. Kyntheum® Summary of Product Characteristics 2017. Available from: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_ Information/human/003959/WC500232913.pdf 6. European Medicines Agency. EPAR summary for the public: Cosentyx. 2015. Available from: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Summary_for_the_public/human/003729/WC500183132. pdf (Accessed July 2017) 7. Taltz®. Summary of Product Characteristics 2016. Available from: http://www.ema.europa.eu/docs/en_GB/ document_library/EPAR_-_Product_Information/human/003943/WC500205804.pdf (Accessed July 2017) 8. Stelara®. Summary of Product Characteristics 2009. Available from: https://www.medicines.org.uk/emc/medicine/32569 (Accessed July 2017) 9. Enbrel®. Summary of Product Characteristics 2000. Available from: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_Information/ human/000262/WC500027361.pdf (Accessed May 2017) 10. Humira®. Summary of Product Charateristics 2003. Available from: https:// www.medicines.org.uk/emc/medicine/31860 (Accessed July 2017) 11. Remicade®. Summary of Product Characteristics 1999. Available from: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_Information/human/000240/WC500050888.pdf (Accessed July 2017) 12. Blauvelt A, et al. Rapid onset of action in patients with moderate-to-severe psoriasis treated with brodalumab: A pooled analysis of data from two phased-3 randomized clinical trials (AMAGINE-2 and AMAGINE-3). J Am Acad Dermatol. 2017; in press 13. Strober B, et al. J Am Acad Dermatol. 2016; 75:77–81 14. Khalid JM, et al. J Dermatolog Treat. 2014;25:67-72 15. Gordon KB, et al. Br J Dermatol. 2014;170:705–15 16. Attia A, et al. Clin Drug Investig.2017; DOI: 10.1007/s40261-017-0500-9 17. Papp K, et al. Br J Dermatol. 2016;175:273–286
RESULTS
Disease factsheet for journalists
CLIENT
Novartis COPD Life is Calling Roadmap
Still Fighting for Breath
About Chronic Obstructive Pulmonary Disease (COPD)
2014 Jul
Asthma Patient Survey
Asthma is a global health problem, 1 affecting 300 million people worldwide. 2 A new large-scale survey of almost 1,333 patients from around the world* revealed uncontrolled asthma is extremely common and restricting lives.3
MILLION PEOPLE
worldwide are living with COPD and the prevalence is rising 2
COPD
COPD
is the world’s fourth leading cause of death3
affects both men and women equally4
88%
Oct
Nov
Dec
2015 Q1
42%
Q3
Phase III Phase III is the pinnacle of the programme. An event that will bring together key stakeholders to seek creative solutions to improve the lives of people with COPD.
Ensure the creation and launch of a successful programme.
Inspire and empowerpatients to speak to their HCP.
Position Novartis as a thought leaders in: COPD, the pharmaceutical industry and business.
Interviews kick-off
self-estimated themselves as controlled, compared to 6% deemed controlled according to clinical guidelines
Q2
Phase II Phase II is the campaign kick-off which will inspire and enable patients to share their personal challenges with the community and their HCP to obtain better care.
Milestones
COPD is a progressive, potentially life-threatening condition that makes it hard to breathe1
reported their condition impacted their daily lives
Sep
Objectives
Headline findings: 3
COPD today
25
Description
Aug
Phase I Phase I will identify key stakeholders to engage throughout the programme. Insights gathered will inform and shape the remainder of the programme.
Website launch
Twitter launch
Facebook page launch
CrOwdshaPeD event
Key online influencers engagement Patients/PAGs/carers/family, HCPs, media, citizen journalists
Tactical Execution
• Novartis values your opinion and would love your input and support (online/offline) in a global patient programme COPD interviews + report Stakeholders (patients/ PAGs/carers/family, HCPs, media, citizen journalists) • Novartis would like you to help inform and shape an exciting global patient programme to change the face of COPD
Website Patients and HCPs • Set your own personal goal and speak to your HCP about how to achieve it • Share your challenge with the global online community to inspire others to join you
• Novartis is facilitating a game-changing event in healthcare • Provide your input and show your support online • Become part of the solution by getting involved on Facebook and Twitter
Facebook page Patients
84% Symptoms
Diagnosis
Most common symptoms are shortness of breath, phlegm, a chronic cough, wheezing and tightness of the chest5
COPD is diagnosed with spirometry10
• Join the global online COPD community to share your experiences, take part in the campaign, support others and improve your QoL
said physical activities were affected by their asthma
34%
Global and local outreach
61%
mild-to-moderate COPD remain undiagnosed
reported they need >24 hours to recover after an asthma attack
50%
Common treatments
Patients/PAGs, HCPs, media, Novartis, stakeholders from other industries • Novartis is a thought leader committed to improving the lives of people with COPD and is investing in discovering innovative solutions to meet patient needs
have reported being diagnosed with a psychological condition because of their asthma
Twitter handle Patients/PAGs, HCPs, media, general public • Novartis is facilitating a game-changing event in healthcare • Provide your input and show your support online • Become part of the solution
Bronchodilators are central to treatment . They work by relaxing and opening air passages in the lungs
Two Kinds (resuce medication) – help to decrease shortness of breath
Long-acting13 used regularly to open the airways and keep them open
• Novartis is a thought leader committed to improving the lives of people with COPD and is investing in discovering innovative solutions to meet patient needs Event
60-85% of people with
Short-acting13
• Novartis is facilitating a game-changing event in healthcare • Provide your input and show your support online • Become part of the solution
Media outreach
• Novartis is encouraging people with COPD to inspire one another by setting themselves personal challenges and sharing them with a global online community • By working with their HCP to achieve these challenges, people with COPD can improve their QoL
Most are not diagnosed until disease is advanced ,
COPD exacerbations worsen disease progression , and increase risk of hospitalization and death8,9
have taken time off work due to their condition
Inhaled corticosteroids recommended for those at high risk of exacerbations, but there
I have to live within my limitations, avoid situations
My asthma completely incapacitates
where my asthma is triggered. I’m not as fit and active as I would like to be anymore.
me. It turns me into a different person.
are health risks with long-term steroid use , , ,
Inhalers may contain either a single or a combination
Inputs
of medication
* Data collected from: References 1. COPD Foundation. What is COPD. https://www.copdfoundation.org/What-is-COPD/Understanding-COPD/What-is-COPD.aspx. Last accessed March 2018. 2. World Health Organization. Chronic Obstructive Pulmonary Disease Fact Sheet. November 2017. http://www.who.int/mediacentre/factsheets/fs315/en/ . Last accessed March 2018. 3. World Health Organization: The top 10 causes of death fact sheet No 310. Available at: http://www.who.int/mediacentre/factsheets/fs310/en/ [Accessed December 2017]. 4. Jenkins CR, Chapman KR, James FD et al.Improving the Management of COPD in Women. Chest 2017; 151(3):686-696 5. COPD Foundation. Signs and Symptoms of COPD. https://www.copdfoundation.org/What-is-COPD/Understanding-COPD/What-is-COPD.aspx. Last accessed March 2018. 6. Wedzicha JA, Seemungal TA. COPD exacerbations: defining their cause and prevention. Lancet 2007; 370(9589): 786-96. 7. Global Initiative for Chronic Obstructive Lung Disease. Pocket guide to COPD diagnosis, management and prevention. A Guide for Health Care Professionals. 2018 Report. http://goldcopd.org/wp-content/uploads/2018/02/WMS-GOLD-2018-Feb-Final-to-print-v2.pdf. 8. Seemungal T et al. Exacerbation rate, health status and mortality in COPD – a review of potential interventions. Int J Chron Obstruct Pulmon Dis. 2009; 4: 203–223. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2699821/# 9. Torabipour A et al. Cost analysis of hospitalized patients with chronic obstructive pulmonary disease: a state-level cross-sectional study. Tanaffos 2016; 15(2): 75-82 https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5127618. 10. Global Initiative for Chronic Obstructive Lung Disease. Diagnosis. Pocket guide to COPD diagnosis, management and prevention. A Guide for Health Care Professionals. 2018 Report. http://goldcopd.org/wp-content/uploads/2018/02/WMS-GOLD-2018-Feb-Final-to-print-v2.pdf. Fromer L. Diagnosing and treating COPD: understanding the challenges and finding solutions. Int J Gen Med. 2011; 4: 729-739. Kaplan W. Background Paper 6.13: Chronic Obstructive Pulmonary Disease (COPD).http://www.who.int/medicines/areas/priority_medicines/BP6_13COPD.pdf. Last accessed April 2018. Pharmacologic therapy for stable COPD. Global Initiative for Chronic Obstructive Lung Disease. Pocket guide to COPD diagnosis, management and prevention. A Guide for Health Care Professionals. 2018 Report. http://goldcopd.org/wp-content/uploads/2018/02/WMS-GOLD-2018-Feb-Final-to-print-v2.pdf. Kew KM, A S. Inhaled steroids and risk of pneumonia for chronic obstructive pulmonary disease. Cochrane Database Syst Rev 2014; 10. Brode SK, Campitelli MA, Kwong JC, et al. The risk of mycobacterial infections associated with inhaled corticosteroid use. Eur Respir J 2017; 50. Suissa S, Kezouh A, Ernst P. Inhaled corticosteroids and the risks of diabetes onset and progression. Am J Med 2010; 123: 1001-1006.
The study enrolled 1,333 adult patients (≥18 years) and children (6-17 years old) suffering from severe persistent asthma. Interviews were conducted between 12th July and 31st October 2016. All data labeled as from adolescent patients were captured through interviews with their caregivers, due to legal restrictions.
Outputs
References: 1. Global Strategy for Asthma Management and Prevention (2017). Available at: http://ginasthma.org/2017-gina-report-global-strategy-for-asthma-management-and-prevention/ [Accessed April 2017]. 2. World Health Organization. Global surveillance, prevention and control of chronic respiratory diseases: a comprehensive approach, 2007. http://www.who.int/gard/publications/GARD%20Book%202007.pdf. [Accessed August 2017] 3. Katsaounou P, Conde L G, Kroegel C et al. The challenges of living with severe asthma in Europe, 2017.
• Insights and content inform the digital strategy • New relationships augment reach and secure success • Report results will shape media outreach • Successful identification of key stakeholders • Quality insights • New relationships with potential for growth
KPIs
Activity
Stakeholders
• Insights and content from Phase I and II define CrOwdshaPeD • User submitted challenges infrom CrOwdshaPeD and media outreach • Online/offline noise builds excitement for CrOwdshaPeD
• Patient submitted challenges • Dwell time/interactions on the patient support web page • Quality of social media interactions • Global media coverage • Participation from key global stakeholders • CPO programme uptake
• 4+ creative solutions to real life COPD patient needs • Potential to help bring the idea to market
• Quality of participants • Quality of solutions • Social media participation • Augmented Novartis SoV (online/offline) • Quality of online and offline coverage
Messaging
Date of Prep: August 2017 Job code: GLRESP/SoM/0003
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Jobcode: xxx | Date of preparation: September 2017
“I have to live with my
limitations, avoid situations where my asthma is triggered. I’m not as fit and active as I would like to be anymore”
The number of new COPD diagnoses is
growing nearly 3X FASTER in women than in men
No. 1 Top tip to prevent attacks:
Relax and take it easy. Stress can cause asthma attacks
88%
Did you know? Your left lung is smaller than your right lung to make room for your heart
http://www.nhlbi.nih.gov/health/health-topics/topics/hlw/system
CLIENT
PROJECT
WORK TYPE
Novartis
Various marketing materials
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
• E-Marketing Designs • PowerPoint Presentations • Infographics
of people reported their condition impacted their daily lives
CLIENT
Novartis womentalkcopd.com
Women Talk COPD WOMEN TALK
COPD Crowdshaped
Avoiding Isolation
A new approach to thinking about COPD
How can I stay active?
How do I talk to my doctor about my breathlessness?
Everyone’s lungs weaken over time, but it happens faster in people who have COPD. As COPD worsens, everyday actions like getting dressed can cause breathlessness.
If at any point you discover a new symptom or if your symptoms get worse, you should call your doctor.
This may make you feel uncomfortable, but you should not be less active because of it. Regular exercise can actually make you feel less breathless over time.
6 Go to physical therapy if recommended by your doctor
Walk around the house
Stay mobile and participate in activities like going for a walk
See how far you can walk in 6 minutes and try to go further next time
• Set a clear goal for your next visit • Monitor how you feel and take your notes to your next visit • Write down any questions and topics you want to discuss with your doctor
During your appointment: • Be assertive and open • Be clear on the problem • Ask for a solution and work with your doctor
After your appointment: • Take time to reflect
Job Number: XXX/XXX/XXXXXX Date of preparation: March 2015
Job Number: XXX/XXX/XXXXXX Date of preparation: March 2015
Eating a healthy diet is important for everyone, especially if you have COPD. The muscles you use for breathing may need 10 times more calories than those of a person without COPD. Here are some things you could do to get the right nutrients while maintaining a healthy weight:
Before your appointment:
Consult your doctor for advice on what you can do to manage your breathlessness
Consult your doctor for advice on what you can do to stay active.
Tips on eating and energy
CLIENT
PROJECT
WORK TYPE
Novartis
Various marketing materials
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Eat high-fiber foods like vegetables and whole grains
Drink non-caffeinated or non-alcoholic drinks
Consult your doctor for advice on healthy eating. Job Number: GLRESP/COPD/0014c Date of preparation: March 2015
• E-Marketing Designs • PowerPoint Presentations • Infographics
Use herbs instead of salt
Stay away from foods that cause bloating (soda or fried foods)
CLIENT
Novartis
COPD & DIAGNOSIS CLINICAL ENDPOINTS
COPD CLINICAL ENDPOINTS CHRONIC OBSTRUCTIVE
PULMONARY DISEASE
Chronic Obstructive Pulmonary Disease (COPD)
(COPD)
is a progressive, life threatening condition characterized by
Common symptoms include:
210 million
Approximately people have COPD
of people with COPD are
Burden of this disease impacts individuals and society:
remains a serious global health problem
There are significant associated direct and indirect healthcare costs
• Chronic sputum/phlegm production
There is an unmet need to optimize the management of
• Chronic cough
COPD
AFFECTS UP TO
Shortness of breath This is the most common symptom of COPD and is persistent3. It is caused by lung inflammation and airflow limitation and worsens over time, particularly with exercise4
• Shortness of breath
less than 65 years old2
COPD
Chronic Obstructive Pulmonary Disease
Symptoms and exacerbations
Who’s affected?
50%
LANTERN STUDY
is a condition characterized by airflow obstruction1
AIRFLOW OBSTRUCTION1
Estimates suggest that
COPD
• Wheeze2
Projected to be the
LAMA
symptoms worsen beyond the day-to-day norm5
COPD treatments aim to reduce symptoms and the future risk of exacerbations, and to improve the quality of life and well-being for the patient5
COMMON SYMPTOMS INCLUDE:
Shortness of breath • Chronic sputum/phlegm production Chronic cough • Wheeze3 The morning is reported as the worst time of the day for shortness of breath making routine activities e.g. showering and getting dressed difficult to complete5
Shortness of breath This is the most common symptom of COPD and is persistent4. It is caused by lung inflammation and
to
airflow limitation
What are the risk factors for
COPD?
Tobacco smoking is one of the major risk factors of COPD1
Other risk factors include smoke from home cooking and heating fuels, occupational dusts, environmental pollution and chemicals or a family history of COPD1
Transition Dyspnea Index (TDI) TDI gives the change in breathlessness severity from a baseline assessment established by the BDI. Ranging from - 9 to + 9, the lower the score, the more deterioration in severity of breathlessness8
If an individual over 40 years old displays any of the symptoms or risk factors associated with COPD, the physician will do a breathing test to measure airflow limitation1
COPD diagnosed in the clinic?
How is
Spirometry
This is a test to measure how WELL a person can blow air out of their lungs (volume) It also measures how FAST a person can blow air out (f low)
A spirometry test is measured by a device called a spirometer and helps diagnose COPD and calculate the severity of the disease:
1 2 3 4 5 6
What are
–
FVC (Forced Vital Capacity) The amount of air that can be forced out after taking a deep breath
FEV1/FVC The ratio of FEV1 to FVC expressed as a percentage and is decreased in patients with COPD6
Trough FEV1 The mean value of FEV1 measured at 24h after the morning doses
Spirometry
Exacerbations contribute to an increased shortness of breath, at times acute and life-threatening, and increases the rate of disease progression for the patient7. It could also result in an unexpected death
COPD treatments aim to reduce symptoms and the future risk of exacerbations, and to improve the quality of life and well-being for the patient7
What clinical endpoints
are measured in
9
9
+
WEEK STUDY
THIS STUDY WAS CONDUCTED IN
Rescue medication use As the use of rescue medication reflects effects on symptoms it can be considered a clinical endpoint. Studies may record the number of times that it is required during the day and at night and the number of puffs per occasion
COPD?
Baseline Dyspnea Index (BDI) BDI evaluates the severity of breathlessness (dyspnea) at a single point in time. Ranging from 0 to 12, the lower the score, the worse the severity of breathlessness8
A spirometry test is measured by a device called a spirometer and helps diagnose COPD and calculate the severity of the disease:
1 2 3
Transition Dyspnea Index (TDI) TDI gives the change in breathlessness severity from a baseline assessment established by the BDI. Ranging from - 9 to + 9, the lower the score, the more deterioration in severity of breathlessness8
4
St. George's Respiratory Questionnaire (SGRQ) This is designed to measure impact on overall health, daily life, and perceived well-being in patients with obstructive airways disease9. Scores are expressed as a percentage of overall impairment where 100 represents worst possible health Rescue medication use As the use of rescue medication reflects effects on symptoms it can be considered a clinical endpoint. Studies may record the number of times that it is required during the day and at night and the number of puffs per occasion
5 6
Exercise endurance Methods for evaluating exercise capacity include 6-min walking test, progressive exercise testing and endurance tests, using a cycle ergometer or treadmill10
FVC (Forced Vital Capacity) The amount of air that can be forced out after taking a deep breath
FEV1 (Forced Expiratory Volume in 1 Second) The amount of air that can be forced out in ONE SECOND after taking a deep breath
FEV1/FVC The ratio of FEV1 to FVC expressed as a percentage and is decreased in patients with COPD6
FEV1 AUCo-4h The change in FEV1 0-4 hours after the morning dose, known as the Area Under The Curve (AUC)9
Trough FEV1 The mean value of FEV1 measured at 24h after the morning doses Peak FEV1 The maximum FEV1 observed
744
Global Initiative for Chronic Obstructive Lung Disease (GOLD). Global Strategy for the Diagnosis, Management, and Prevention of Chronic Obstructive Pulmonary Disease. Updated 2013. Available at: http://www.goldcopd.org/guidelines-global-strategy-for-diagnosis-management.html [Accessed 17 July 2014]
2
Fletcher MJ et al. COPD Uncovered: An International Survey on the Impact of Chronic Obstructive Pulmonary Disease (COPD) on a Working Age Population. BMC Public Health 2011;11:612
3
Partridge MR et al. Patient Insight into the Impact of Chronic Obstructive Pulmonary Disease in the Morning: an internet survey. Curr Med Res Opin 2009;25(8):2043-2048
4
Pitta F, Troosters T, Spruit MA, et al. Characteristics of Physical Activities in Daily Life. Am J Respir Crit Care 2005;171:972–977. Available at: http://www.atsjournals.org/doi/pdf/10.1164/rccm.200407-855OC [Accessed 17 July 2014]
5
Joshi M et al. Symptom Burden in Chronic Obstructive Pulmonary Disease and Cancer. Curr Opin in Pulm Med 2012;18(2):97–103
6
Spirometry in Practice. Available at: https://www.brit-thoracic.org.uk/document-library/delivery-of-respiratory-care/spirometry/spirometry-in-practice/ [Accessed 17 July 2014]
7
Vestibo J et al. (2012). Global Strategy for the Diagnosis, Management and Prevention of Chronic Obstructive Pulmonary Disease, GOLD executive summary [published online ahead of print August 9, 2012]. Am J Respir Crit Care Med. doi: 10.1164/rccm.201204-0596PP. [Accessed 17 July 2014]
8
American Thoracic Society. Available at: http://www.thoracic.org/assemblies/srn/questionaires/bdi-tdi.php [Accessed 17 July 2014]
9
American Thoracic Society. Available at: http://www.thoracic.org/assemblies/srn/questionaires/sgrq.php [Accessed 17 July 2014]
ACROSS
Lantern met both primary and key secondary endpoints
Ultibro Breezhaler demonstrated non-inferiority vs Seretide Accuhaler in terms of trough FEV1 at Week 267 Results showed
superiority of Ultibro Breezhaler in improving lung function
(as measured by trough FEV1) compared to the Seretide Accuhaler at week 267
Ultibro Breezhaler significantly reduced the rate of moderate-to-severe exacerbations by
1.
Global Initiative for Chronic Obstructive Lung Disease (GOLD). Global Strategy for the Diagnosis, Management, and Prevention of Chronic Obstructive Pulmonary Disease. Updated 2013. Available at: http://www.goldcopd.org/guidelines-global-strategy-for-diagnosis-management.html [Accessed 17 July 2014]
2.
Partridge MR et al. Patient Insight into the Impact of Chronic Obstructive Pulmonary Disease in the Morning: an internet survey. Curr Med Res Opin 2009;25(8):2043-2048
3.
Pitta F, Troosters T, Spruit MA, et al. Characteristics of Physical Activities in Daily Life. Am J Respir Crit Care 2005;171:972–977. Available at: http://www.atsjournals.org/doi/pdf/10.1164/rccm.200407-855OC [Accessed 17 July 2014]
4.
Joshi M et al. Symptom Burden in Chronic Obstructive Pulmonary Disease and Cancer. Curr Opin in Pulm Med 2012;18(2):97–103
5.
Vestibo J et al. (2012). Global Strategy for the Diagnosis, Management and Prevention of Chronic Obstructive Pulmonary Disease, GOLD executive summary [published online ahead of print August 9, 2012]. Am J Respir Crit Care Med. doi: 10.1164/rccm.201204-0596PP. [Accessed 17 July 2014]
6.
American Thoracic Society. Available at: http://www.thoracic.org/assemblies/srn/questionaires/bdi-tdi.php [Accessed 17 July 2014]
7.
American Thoracic Society. Available at: http://www.thoracic.org/assemblies/srn/questionaires/sgrq.php [Accessed 17 July 2014]
8.
Oga T et al. Exercise responses during endurance testing at different intensities in patients with COPD. Respiratory Medicine 2004; 98:515–521
9.
Spirometry in Practice. Available at: https://www.brit-thoracic.org.uk/document-library/delivery-of-respiratory-care/spirometry/spirometry-in-practice/ [Accessed 17 July 2014]
PROJECT
WORK TYPE
Novartis
Various marketing materials
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
31% **
7
Exacerbations are categorised by severity according to need for additional treatment. * The LANTERN study used Seretide (salmeterol/fluticasone) 50/500 mcg, which is indicated in the UK for the symptomatic treatment of patients with COPD, with a FEV1 <60% predicted normal (prebronchodilator) and a history of repeated exacerbations, who have significant symptoms despite regular bronchodilator therapy8. The patient population in the LANTERN study were moderate-to-severe COPD patients with or without (≤1) exacerbation in the previous year7. Seretide is also known as Advair® and Accuhaler is also known as Diskus®. Seretide, Advair, Diskus and Accuhaler are registered trademarks of the GlaxoSmithKline group of companies.
References:
References:
CLIENT
56 sites
** RR [95% CI]: 0.69 [0.48, 1.00]; p=0.048)
10 Oga T et al. Exercise responses during endurance testing at different intensities in patients with COPD. Respiratory Medicine 2004; 98:515–521 11 EMA. Guideline on clinical investigation of medicinal products in the treatment of chronic obstructive pulmonary disease (COPD). 21 June 2012. Available at: http://www.ema.europa.eu/docs/en_GB/document_library/Scientific_guideline/2012/08/WC500130880.pdf [Accessed 17 July 2014]
at
Argentina, Chile, China and Taiwan6
1.
Global Alliance Against Chronic Respiratory Disease (GARD). Global Surveillance, Prevention and Control of Chronic Respiratory Disease: a Comprehensive Approach. Available at: http://www.who.int/entity/gard/publications/GARD%20Book%202007.pdf?ua=1 [Accessed 17 July 2014]
2.
Global initiative for Chronic Obstructive Lung Disease (GOLD). Global Strategy for the Diagnosis, Management, and Prevention of Chronic Obstructive Pulmonary Disease. Updated 2014. Available at: http://www.goldcopd.org/uploads/users/files/GOLD_Report_2014_Jun11.pdf [Accessed 17 July 2014]
3.
EMA. 2012. Ultibro Breezhaler EU Summary of Product Characteristics. [Online] 3 October 2013. Available at: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_Information/human/002679/WC500151255.pdf [Accessed 17 July 2014].
References: 1
assessing the efficacy and safety of Ultibro Breezhaler vs Seretide® Accuhaler®* in patients with moderate-to-severe COPD, with or without a history of moderate-to-severe exacerbations (worsening symptoms) in the previous year6
26
St. George's Respiratory Questionnaire (SGRQ) This is designed to measure impact on overall health, daily life, and perceived well-being in patients with obstructive airways disease7. Scores are expressed as a percentage of overall impairment where 100 represents worst possible health
This is a test to measure how well a person can blow air out of their lungs (volume) It also measures how fast a person can blow air out (flow)
Patients with exacerbations are at an increased risk of hospitalization and often require a change in medication1
is a once-daily maintenance bronchodilator treatment approved in the EU to relieve symptoms in adult patients with COPD3
was a
Diagnosis
COPD exacerbations?
Ultibro® Breezhaler®
Breezhaler®inhalation device allows patients and see hear , feel
was a
Peak FEV1 The maximum FEV1 observed
Exacerbations are when a patient’s respiratory symptoms worsen beyond the
Questionnaires and other measures are often used to assess the overall impact of COPD on the patient’s quality of life, for example:
9
+
LABA indacaterol
LANTERN LANTERN
Exercise endurance Methods for evaluating exercise capacity include 6-min walking test, progressive exercise testing and endurance tests, using a cycle ergometer or treadmill8
FEV1 AUCo-4h The change in FEV1 0-4 hours after the morning dose, known as the Area Under The Curve (AUC)6
day-to-day norm7
–
9
FEV1 (Forced Expiratory Volume in 1 Second) The amount of air that can be forced out in ONE SECOND after taking a deep breath
+ +
that they have taken the full treatment correctly 4,5
Baseline Dyspnea Index (BDI) BDI evaluates the severity of breathlessness (dyspnea) at a single point in time. Ranging from 0 to 12, the lower the score, the worse the severity of breathlessness6
Questionnaires and other measures are often used to assess the overall impact of COPD on the patient’s quality of life, for example:
3rd
The
Clinical endpoints
and worsens over time, particularly with exercise5
leading cause of 2
glycopyrronium bromide
COPD symptoms?
people worldwide1
3rd DEATH by 2020
Exacerbations are when a patient’s respiratory What are
210 million
4.
Pavkov et al. Characteristics of a Capsule Based Dry Powder Inhaler for the Delivery of Indacaterol. CMRO 2010;26;11:2527-2533
5.
Onbrez® Breezhaler® (indacaterol) EU Summary of Product Characteristics. [Online] July 26, 2012 Available at: http://www.ema.europa.eu/docs/en_GB/document_library/EPAR_-_Product_Information/human/001114/WC500053732.pdf [Accessed 17 July 2014]
6.
Clinicaltrials.gov. A 26-week Treatment Randomized, Double-blind, Double Dummy Study to Assess the Efficacy and Safety of QVA149 (LANTERN). NCT01709903. Available at: http://clinicaltrials.gov/ct2/show/NCT01709903 [Accessed 17 July 2014]
7.
Zhong N et al. Efficacy and safety of once-daily QVA149 compared with twice-daily salmeterol/fluticasone combination (SFC) in patients with COPD: the LANTERN study. [ERS abstract 700090; Session 281; Date: September 8 2014; Time].
8.
Seretide® Summary of Product Characteristics [Online] Available at: https://www.medicines.org.uk/emc/medicine/2317/SPC/Seretide+100,+250,+500+Accuhaler [Accessed 17 July 2014]
• E-Marketing Designs • PowerPoint Presentations • Infographics
CLIENT
Health Unlimited
Open Source
Innovation
osi = zmp?
When
Zeitgeist, MIT and Pharma Collide
Date & Time: 16:00 - 16:45, Sunday, June 19, 2016 Stage: Inspiration Stage Session Holder: Health Unlimited Title: Open Source Innovation When Zeitgeist, MIT and Pharma Collide
Chair: Yossi Vardi, Internet Investor, Entrepreneur Speaker(s): Dr Jack Kreindlier, Founder and Chairman, Sentrian, Remote Patient Intelligence Mark Lightowler, Head of Digital Solutions, Novartis Matt Lowe, Director, Health Unlimited Tal Achituv, Entrepreneur, a full-stack engineer and a seasoned CTO, MIT Media Lab
Open Source
Innovation When
Zeitgeist, MIT and Pharma Collide
CLIENT
PROJECT
WORK TYPE
Health Unlimited
OSI internal event
•
New Business Visualisations
regimen providing clinically-proven support for anyone suffering from thinning hair. Backed by world-class research and scientifically proven to deliver results, TRX2® products are discreet and easy-to-use, delivering thicker, healthier hair without compromise.
CLIENT
Oxford Biolabs
THE BUILDING BLOCKS OF HEALTHY-LOOKING HAIR TRX2® Molecular Food Supplements for Hair are based on natural ingredients and have been specifically designed for men and women suffering from the early stages of hair loss. Packed with all the nutrients needed to maintain a healthy-looking head of hair, including:
YOUR ROOT TO HEALTHIER LOOKING HAIR HAIR LOSS WILL AFFECT 50% OF PEOPLE AT SOME POINT DURING THEIR LIFETME.
Carnitine-L-tartrate
Biotin
Studies show that L-carnitine-L-tartrate promotes human hair growth by increasing the energy supply to the hair.
A deficiency in biotin intake can cause brittle hair and can lead to hair loss. A single boiled egg contains 25 µg of biotin. TRX2® has 150 µg of biotin in a serving – 3 capsules – meaning you would need to eat 6 eggs every day in order to get the same amount.
A portion of red meat provides around 162 mg of L-carnitine-L-tartrate per serving. TRX2® contains 800 mg of L-carnitineL-tartrate in a serving – 3 capsules – meaning you would need to eat meat five times a day to experience the same benefits.
x5 Male-pattern baldness is the most common type of hair loss. It affects around half of all men by 50 years of age1
x6
Around half of women over the age of 70 experience female-pattern baldness2
HAIR GROWTH Hair is the fastest growing tissue in the human body, with most people having between 100,000 and 120,000 strands.3 Optimal growth occurs from age 15 – 30. Hair growth reduces from age 40 - 50.
Promoting new hair growth Regular scalp massages are a great way of boosting hair health, and can simultaneously improve circulation and reduce stress. Follow our guide for the ultimate massage:
Zinc
Selenium
Zinc conditions the hair and helps prevent shedding. Chickpeas, pumpkin seeds, cashews and chicken are all good sources of zinc.
Selenium is needed for a healthy scalp. Nuts, some oily fish, turkey and spinach are all good sources of selenium. A 75g serving of salmon contains 81.15 µg of selenium. TRX2® contains 75 µg of selenium in a serving – 3 capsules – meaning you would need to have salmon for dinner every day for the same effects.
TRX2® contains 15 mg of zinc in a serving – 3 capsules – the same as two cups of cashew nuts.
3-4 1
2
*
x7
x2
times
Hair can be wet or dry, Spread your fingers, Extend and contract but should be clean. If placing fingertips on INFORMATION the fingers three or CONSUMER your hair is wet comb your scalp – avoid using four times, then Please read the consumer information thata comes with TRX2® Hair Revitalizing Lotion (hereinafter referred to as TRX2® through first. You may your fingernails, as they move to different before you start using it. also want to add some can break theLotion) hair and spot and repeat. TRX2® HAIR If you have questions regarding application of this product, contact us at support@trx2.com or +44 800 808 5251. conditioner or hair lotion* damage the scalp. REVITALIZING LOTION For more information on TRX2® Products or to reorder visit our homepage: www.trx2.com.
3
Full range of products available from www.trx2.com
TRX2® Hair Revitalizing Lotion with TRX2® active ingredients is a topical, natural-based solution containing a propriWhat is TRX2® Lotion? Hair Revitalizing Lotion - £42.36 per bottle etary complex of Carnipure™ Tartrate (L-Carnitine Tartrate), Potassium, BCAA, Niacin and other essential nutrients,
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Who may use TRX2®
USE
TRX2® Lotion is suitable for use by men and women. This natural-based solution is specifically designed to revitalize
hair and nourish thinning hair. Lotion? TRX2®: HAIR HEALTH & follicles CONFIDENCE
Created with the expertise of Oxford Biolabs is thinning a safe,hair natural hair loss a decline in potassium channel activity. These pore formPeople whoTRX2® experience often demonstrate How does scientists, ing proteins, which reside in the cell membranes, are responsible for the correct transport of potassium ions over the TRX2® Lotion work? regimen providing clinically-proven support for anyone suffering from thinning hair. Backed thusresults, maintaining the membrane potential by world-class research and scientifically provenmembranes, to deliver TRX2® products are and a normal uptake of nutrients by the hair follicle. TRX2® Lotion is based on the same effective formula as the TRX2® Molecular Food Supplement for Hair. This means that the discreet and easy-to-use, delivering thicker,same healthier hair without compromise. active ingredients help to strengthen the hair by ensuring a sufficient nutrient supply to the hair root. This can
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How should I apply TRX2® Lotion?
When using TRX2® Lotion for the first time, remove the cap. Insert the dropper into the bottle. Squeeze the bulb and release it, allowing the dropper to fill with 1ml of the product. Part your dry, or towel dry, hair in the area of thinning hair. Apply TRX2® Lotion using the tip of the dropper directly onto the part of the scalp you want to treat. Squeeze the bulb slowly to achieve gradual solution release. Apply small amounts of solution to prevent it from running off the scalp. Use your fingers to massage TRX2® Lotion into the scalp. Wash your hands well afterwards. Blow dry or style your hair only after the product has been completely absorbed into your scalp. Allow enough time to dry your hair before going TRX2® Molecular Food Supplements for Hair aretobased onTRX2® natural andfor have bed. Allow Lotioningredients to stay on your scalp a few hours before washing your hair. Apply TRX2®from Lotionthe twiceearly a day, stages in the morning and in the evening. To ensure long-term results, use TRX2® Lotion conbeen specifically designed for men and women suffering of hair loss. sistently as part of your daily routine, and according to the instructions.
THE BUILDING BLOCKS OF HEALTHY-LOOKING HAIR
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Carnitine-L-tartrate
Does TRX2® Lotion contain any harmful ingredients?
Use the usual amount of TRX2® Lotion the next morning or evening. Keep out of reach of children. Store at room temperature. In case of contact with eyes, rinse immediately with cool water.
Biotin TRX2® Lotion is dermatologically tested and doesn’t contain any harmful ingredients. It is free from synthetic fragrances and dyes. Active ingredients of TRX2® Lotion (see label) are natural-based. A small dosage of a mild preservative is used to prevent product spoilage.
Studies show that L-carnitine-L-tartrate A deficiency in biotin intake can cause brittle promotes human hair growth by increasing and can lead to Propanediol, hair loss. Phenoxyethanol, Biotin, Leucine, Isoleucine, Valine, Niacin, Potassium Chloride, Aqua, Carnitine Tartrate, Ingredients: hair Zinc Citrate, Dimethyl Sulfone. the energy supply to the hair. A single boiled egg contains 25 µg of biotin. Dermatologically tested. A portion of red meat provides around TRX2®Free hasfrom 150 µg of biotin in a serving – 3 synthetic frangrances and dyes. 162 mg of L-carnitine-L-tartrate per serving. capsules – meaning you would need to eat 6 TRX2® contains 800 mg of L-carnitineeggs everyend: daysee inbottom orderoftobottle. get the same Best before Specifications: 60 ml. L-tartrate in a serving – 3 capsules – amount. Manufactured for and distributed by: Information updated: November 2015 meaning you would need to eat meat five times a day to experience the same benefits.
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support@trx2.com
per jar
Full range of products available from www.trx2.com References
CLIENT
PROJECT
WORK TYPE
Oxford Biolabs
Various marketing materials Selenium
• Editorial Layouts • E-Marketing Designs
Zinc
Zinc conditions the hair and helps prevent shedding. Chickpeas, pumpkin seeds, cashews and chicken are all good sources of zinc. TRX2® contains 15 mg of zinc in a serving – 3 capsules – the same as two cups of cashew nuts.
x2
1. http://www.nhs.uk/Conditions/Hair-loss/Pages/Introduction.aspx and Otberg N, Finner AM, Shapiro J. Androgenetic alopecia. Endocrinol Metab Clin North Am 2007; 36: 379–98. 2. International Journal Of Trichology [serial online]. July 2016;8(3):116-120. Available from: Academic Search Elite, Ipswich, MA. Accessed February 20, 2017.) 3. S. Bouabbache, A. Galliano, P. Littaye. M/ Leportier, F. Pouradier, E Gillot, S. Panhard, G. Loussouarn, What is a Caucasian ‘fine’ hair? Comparing instrumental measurements, self-perceptions and assessments from hair experts. Volume 38, Issue 6. December 2016, Pages 581–588
Selenium is needed for a healthy scalp. Nuts, some oily fish, turkey and spinach are all good sources of selenium. A 75g serving of salmon contains 81.15 µg of selenium. TRX2® contains 75 µg of selenium in a serving – 3 capsules – meaning you would need to have salmon for dinner every day for the same effects.
x7
CLIENT
Sunovian
Expert Panel Report
port_14_
ellence
iatry 20
at http://
Health Care
No Mental Health Care Without Physical Health Care Executive summary In what has been described as a national scandal,1 people with schizophrenia die 10-20 years earlier on average than the general population.2,3 An estimated 60% of this is due to physical health issues,4 and preventing premature mortality in people with schizophrenia and other severe mental illness (SMI) is now a national priority.5 Numerous publications aimed at addressing this have appeared recently including a national strategy, recommendations for policy makers, evidence-based practice guidelines and NHS indicators and incentives. However, there is a limited supply of practical advice and recommendations to help practising healthcare professionals make a real difference for people with schizophrenia now. To address this gap, a Panel of national experts has developed a series of steps that can be implemented immediately at the clinical level in both secondary and primary care as appropriate. Broader considerations of how to make optimal use of other community services that can promote physical and mental wellbeing are also included, and may enable local teams to make use of innovative services and approaches that are appearing in many parts of the UK. The recommendations cover four key areas of critical need, in which real change can be driven relatively easily and cheaply by local teams working together with commissioners:
1. Adopt a patient-centred approach starting with a holistic assessment of the needs of a person with schizophrenia 2. Ensure people with schizophrenia receive regular physical health assessments and intervene when necessary 3. Develop an integrated service to promote physical health in people with schizophrenia, there is no one-size-fits-all approach 4. Continuity of care and message – consider who engages with the person in their care and makes their experience as streamlined and simple as possible Underneath these themes the Panel has developed recommendations and practical advice to help implement change, as well as providing best practice case studies and listening tools and guidance available to help local care teams. It is hoped that this report will help in some way to bridge the gap between the wider systemic changes that need to happen to ensure parity of outcomes for people with schizophrenia, and the pressing need to drive meaningful changes for people affected by physical health problems now.
On average, people with schizophrenia can expect to die 10-20 years before people without a SMI, with cardiovascular disease being the leading cause of mortality.2,3 NHS England has committed to reducing this gap, including it as an indicator in the NHS Outcomes Framework and incorporating financial incentives into its Commissioning for Quality and Innovation (CQUIN) framework for 2014-15.
No Mental Health Care Without Physical Health Care
Job Code: XXXXXXX | Date of preparation: October 2014 | 1
A 2012 audit of over 5,000 mental health patients found that fewer than 29% receive the basic annual physical health checks and ongoing monitoring support they need.9
Change is coming? NHS outcomes measures for physical health in people with SMI defined At the time of writing real change does appear to be forthcoming, with the Department of Health and NHS England taking more concrete steps to drive behaviour change. In November 2013 the new NHS Outcomes Framework, the mechanism by which the success of the NHS is judged, was published. It now includes a specific indicator for physical health in people with SMI (1.5 Reducing premature death in people with SMI) and a number of related indicators such as Reducing premature death due to cardiovascular disease and Improving quality of life for people with a SMI. This now requires health providers to demonstrate that they are delivering against these indicators and achieving measurable change.10 In February 2014, NHS England went further when it published its 2014-15 Commissioning for Quality and Innovation (CQUIN) framework. The new framework provides financial incentives for NHS trusts to take a more proactive approach to physical health care for people with SMI, and includes two relevant indicators for the 2014-25 financial year: • Indicator 1: 65 % of funding for demonstrating, through a national audit process similar to the National Audit of Schizophrenia, full implementation of appropriate processes for assessing, documenting and acting on cardio-metabolic risk factors in patients with psychoses, including schizophrenia • Indicator 2: 35 % of funding for completion of a programme of local audit of communication with patients’ GPs, focusing on patients on the Care Programme Approach (CPA), demonstrating by Quarter 4 that, for 90 % of patients, an up-to-date care plan has been shared with the GP, including the holistic components set out in the CPA guidance
And finally, in September this year, the Chief Medical Officer for England, published her annual report with focus on ‘Public Mental Health Priorities: Investing in the Evidence’, within which a number of recommendations in the mental health arena are made that are based on and reinforced by the above proposals. These include:
29% Evidence-based guidance and the first steps towards system-level changes NICE published its revised Schizophrenia Clinical Guideline (CG178) in March 2014. This made a number of evidence-based recommendations aimed at improving the physical health of people with schizophrenia. Please see box out for key recommendations. In May the BMA published a comprehensive report entitled Recognising the Importance of Physical Health in Mental Health and Intellectual Disability, which aimed to help the medical profession to drive change. Its recommendations focus on providing parity of esteem for people with mental health problems and intellectual disability, and focus on key areas such as promoting prevention strategies, delivering joined-up care and ensuring adequate training is provided for healthcare professionals.11 This report included an example pathway for an integrated physical care service for people with SMI. The pathway was developed by Rethink Mental Illness in collaboration with the Royal College of General Practitioners, Royal College of Nursing and the Royal College of Psychiatrists. The pathway is available to download here: http://www.rethink.org/about-us/health-professionals/physical-healthintegrated-physical-health-pathway
Getting to the heart of the matter – why this report is necessary Behind all the statistics and talk of systemic change, a large number of people living with schizophrenia need significant and immediate change in the clinical care they receive. This report is designed to represent a natural ‘next step’ to the performance indicators and evidence base through providing practical steps that can be taken now. While the political will to deliver change is clear and evidence-based interventions exist, there remains a lack of practical help and advice for local care teams who are committed to driving change in their area. This report builds on the work of others and the experience of experts in the field to create a set of practical recommendations that can help implement NICE guidance, achieve CQUIN targets and, most importantly of all, provide increased longevity and quality of life to people living with schizophrenia.
• All Health and Wellbeing Boards being informed by a Joint Strategic Needs Assessment (JSNA) which includes the information needed to plan services to integrate the mental and physical health needs of their populations • The Outcomes Frameworks working together to develop a metric that recognises patient experience of the integration of their care and leads to rewards for effective integration around the patient’s health and social care needs • The Mental Health Intelligence Network linking routine mental health data to longitudinal mental health survey data to better understand patterns of mental illness across the community, including those affected by the 75% treatment gap • Ensuring a period of specific mental health training in GP training
A further example care pathway can be found within the Lester UK adaptation. It outlines an intervention framework for people experiencing psychosis and schizophrenia. The resource was co-produced by NHS England, NHS Improving Quality, Public Health England and the National Audit of Schizophrenia Team, and is available for download here: http://www.rcpsych.ac.uk/quality/NAS/resources
4 | Job Code: XXXXXXX | Date of preparation: October 2014
CLIENT
PROJECT
WORK TYPE
Sunovian
Various marketing materials
• Editorial Layouts • E-Marketing Designs • Infographics
The report is available for download here: https://www.gov.uk/government/uploads/system/ uploads/attachment_data/file/351629/Annual_ report_2013_1.pdf No Mental Health Care Without Physical Health Care
No Mental Health Care Without Physical Health Care
Job Code: XXXXXXX | Date of preparation: October 2014 | 5
CLIENT
Takeda
UN
TRE
A AT E D s
Controversies and Progress in T-Cell Lymphoma Including a preview of the 2021 BSH T-cell guidelines 12th November 2020 | 8:00am – 9:30am This symposium with Dr Graham Collins, Dr Matthew Ahearne, Dr Chris Fox and Professor Tim Illidge will be taking place tomorrow on the 12th November from 8:00am – 9:30am. Please find the agenda below:
ADCETRIS
®
Time
Session
Speaker
8:00 – 8:05
Introduction
Dr Graham Collins
8:05 – 8:20
T-Cell Lymphoma – A Moving Target
Dr Graham Collins
8:20 – 8:35
Towards Molecularly-Guided Therapy for TNHL
Dr Matthew Ahearne
8:35 – 8:50
Guidelines Update – Controversies & Progress
Dr Chris Fox
8:50 – 9:15
Challenging Clinical Cases – Ask the Experts
Professor Tim Illidge
9:15 – 9:30
Q&A Meeting Close
All Dr Graham Collins
brentuximab vedotin
Your treatment and what to expect from it Information for people who have been prescribed ADCETRIS (brentuximab vedotin) for Hodgkin lymphoma, systemic anaplastic large cell lymphoma or cutaneous T-cell lymphoma.
We look forward to welcoming you to what we anticipate will be a thought-provoking and informative symposium. If you have any questions, please don’t hesitate to contact: Steve Meredith Takeda Oncology Key Account Manager West Midlands
Tory Griffiths Takeda Oncology Key Account Manager Manchester & Merseyside
This booklet does not replace your healthcare professional’s advice. Always ask your doctor, nurse or pharmacist any questions you might have about your treatment or disease.
Geeta Menon Takeda Oncology Key Account Manager East Midlands & Anglia
ADCETRIS in combination with CHP is indicated for adult patients with previously untreated sALCL.2 ADCETRIS has received a conditional marketing authorisation in Europe. Prescribing information can be found on the last page.
Takeda medicines will be discussed during this meeting. This sponsored symposium is organised and fully funded by Takeda UK Ltd. and is intended for healthcare professionals only as part of the BSH 2020 annual conference. Prescribing information will be available during this meeting.
Please refer to the patient information leaflet for brentuximab vedotin. In the UK it can be found at www.medicines.org.uk/emc/product/2859/pil. In Ireland it can be found at www.medicines.ie/medicines/adcetris-50-mgpowder-for-concentrate-for-solution-for-infusion-31191/patient-info.
C-APROM/UKI/ADCE/0007 | October 2020
Mepact demonstrated a predictable, manageable tolerability profile1,2
NICE sALCL background Study design Study design
When used in combination with chemotherapy, Mepact was shown to have mild to moderate side effects.2 These were largely related to immune activation and the resulting biological activity.1- 3
Population Efficacy Tolerability
Hearing loss was the only AE that occurred at a higher frequency with Mepact in combination with chemotherapy, versus chemotherapy alone.1
Dosing Summary
See ALK+ aNSCLC, Think Brain Metastases, Choose ALUNBRIG (brigatinib)
MEETINGS SUMMARY
UNDERSTANDING COMMON ENDPOINTS AND TERMINOLOGY IN LUNG CANCER CLINICAL TRIALS
HIGHLIGHTS
Trial design
Reported endpoints
For both intracranial and extracranial efficacy1 Up to 90% of ALK+ aNSCLC patients will develop brain metastases during their disease.2
Treatment decision
Patients need a treatment that delivers both intracranial and extracranial efficacy.
N=? PFS
OS
ORR
QOL
iPFS
DOR
Cross-over Single-arm
With your help, these sessions were lively and engaging exchanges, in which we explored and interrogated the latest developments in lung cancer research from the 2018 WCLC and ESMO conferences. By linking research developments to how they might improve outcomes for lung cancer patients and impact clinical practice in the UK, we hope you found these sessions to have relevance to your current and future clinical practice.
Randomised
Please take the time to watch the key takeaways from the meetings, as summarised by our expert panel below
Inclusion/ exclusion
Phase
Interventional/ observational
Comparator arm
?
ALUNBRIG has a generally manageable tolerability profile
• Halved the risk of disease progression or death vs crizotinib in ITT population (BIRC-assessed mPFS of 24.0 months with ALUNBRIG vs 11.0 months with crizotinib, HR=0.49; P<0.0001)1
• In the ALTA-1L study, the most common (>25%) AEs of any grade included diarrhoea, increased blood CPK, cough, hypertension, nausea, and increased AST1
• Two thirds reduction in risk of intracranial disease progression or death in patients with any brain metastases at baseline (BIRCassessed intracranial mPFS of 24.0 months with ALUNBRIG vs 5.6 months with crizotinib, HR= 0.31; P<0.0001)1
Patients should be provided with a Patient Alert Card when prescribed ALUNBRIG.
What do these endpoints mean?
CON
OVERALL SURVIVAL (OS), PROGRESSION-FREE SURVIVAL (PFS) AND DURATION OF RESPONSE (DOR)1
GENE RA TO LLY LE M RA
BLE EA AG Y1 ANILIT B
1 D CY AN ICA IC FF M LE A
E1
Primary endpoint
Thank you for attending one of the Takeda Oncology organised HIGHLIGHTS: WCLC and ESMO Lung Cancer Updates held last year in London and Manchester.
ALUNBRIG provided superior systemic and intracranial efficacy vs crizotinib1
VE
LIF
Dear healthcare professional,
INTRA SYS CR TE AN I
LUNG CANCER UPDATES
Wednesday 5th December 2018 Cheltenham Suite, Manchester Airport Marriott Hotel
Clinical interpretation
WCLC & ESMO
Death
N
DOR We are also pleased to announce that, due to the success of these meetings, we are looking to hold similar sessions following the 2019 conferences later this year. So please make sure you keep an eye out for further correspondence, and we hope to see you at a future HIGHLIGHTS meeting.
Advantages1 OS
Yours sincerely,
PFS
Takeda Oncology Medical Department
DOR Job code: XXX | Date of preparation: March 2019
Disadvantages1
• Considered the gold standard in lung cancer trials2 • Easily and precisely measured • Completely objective
• Often affected by crossover and/or subsequent therapies • Needs long follow-up to get enough events • Includes non-cancer deaths
• Generally assessed earlier than OS • Requires a smaller number of trial participants than OS • Not influenced by crossover and subsequent therapies
• Potentially influenced by assessment bias • May be confounded by frequency of radiological or other assessments • May not correlate highly with survival
• Can reflect fast onset of treatment efficacy • Can highlight a plateau in response
• Only based on a subset of patients (responders)3 • May not be balance of baseline characteristics3
DO
SIN
G1
ALUNBRIG comes with a convenient dosing schedule
Until disease progression or cancer death
PFS
T
NICE RECOMMENDED TREATMENT OPTIONS IN ALK-POSITIVE ADVANCED NSCLC A GUIDE FOR HEALTHCARE PROFESSIONALS
OF
Disease progression
E
Documentation of tumour response
NI
Randomisation or enrolment OS
• The only licensed first-line treatment for ALK+ aNSCLC that has a single tableta,once-daily dosing regimen3–6
QU
AL
IT
Y
ALUNBRIG delivered a sustained and significantly longer duration of improvement in quality of life vs crizotinib1 • Median duration of improvement in GHS/QOL not reached with ALUNBRIG vs 12 months for crizotinib (HR=0.27; P<0.0001)1,7
INDICATIONS3 • ALUNBRIG is indicated as monotherapy for the treatment of adult patients with anaplastic lymphoma kinase (ALK)-positive advanced non-small cell lung cancer (NSCLC) previously not treated with an ALK inhibitor.
Alunbrig is indicated as monotherapy for the treatment of adult patients with anaplastic lymphoma kinase (ALK)-positive advanced non-small cell lung cancer (NSCLC) previously not treated with an ALK inhibitor.1 Alunbrig is indicated as monotherapy for the treatment of adult patients with ALK‑positive advanced NSCLC previously treated with crizotinib.1 Please refer to the Summary of Product Characteristics for full prescribing and monitoring guidance.1 For more information, please visit www.ALUNBRIG.co.uk (for UK use only)
• ALUNBRIG is indicated as monotherapy for the treatment of adult patients with ALK-positive advanced NSCLC previously treated with crizotinib. In circumstances where dose is modified from the recommended dose, more than one tablet may need to be taken.
a
CLIENT
PROJECT
WORK TYPE
Takeda Oncology
Isell detail aid Marketing materials Virtual Expo
• Editorial Layouts • New Business Visualisations • E-Marketing Designs • PowerPoint Presentations • Infographics
UK/BRIG/1905/0037a(2) Date of preparation: June 2020
CL
RECOMMENDED IN
ADCETRIS® (brentuximab vedotin) with cyclophosphamide, doxorubicin and prednisone (CHP) is recommended by NICE, within its marketing authorisation, as an option for untreated systemic anaplastic large cell lymphoma (sALCL) in adults.1
L
CLIENT
Takeda
Menu
Menu
ADCETRIS + CHP demonstrated improvement in PFS* vs. CHOP in patients with previously untreated sALCL1,2†
sALCL is clinically aggressive and associated with poor outcomes1,2 References
NICE First-line treatment of sALCL has typically been multi-agent chemotherapy, such as CHOP or CHOP-like regimens4–6
sALCL background
ADCETRIS + CHP provided PFS benefit vs. CHOP regardless of consolidative therapy3*
Abbreviations
Percentage of Progression-Free Patients (%)
PI
— Consolidation of the initial response by means of ASCT to prevent relapse is sometimes used5,7
Study design
• UK guidelines (2011) recommend initial treatment with CHOP for ALK– sALCL (if clinical trial is not an option) and for ALK+ sALCL4
Population
Most clinical practice guidelines recommend inclusion in clinical trial as the preferred first-line option for sALCL, highlighting the need for novel therapies4–6
Efficacy Typical treatment pathway4–6
Tolerability
Clinical trial (preferred)
If no response or relapse
Second-line therapy
Response
ASCT
Multi-agent chemotherapy
90
70
The benefit of ADCETRIS + CHP vs. CHOP was seen both with and without censoring patients in both treatment groups who received consolidative ASCT therapy3
60 50 40 30 N
20 10 0
Events Median, months
ADCETRIS + CHP 162
47
CHOP 154
70
0
ADCETRIS + CHP 162 CHOP 154
Summary
PI
80
55.7
HR (95% CI)
P-value (nominal)
0.58 (0.40, 0.84)
0.0032
27.1
6
12
18
24
101 85
85 71
75 65
61 50
30
36
42
48
54
60
66
21 28
13 15
4 5
2 1
0 0
ADCETRIS + CHP reduced the risk of a PFS event by 42% compared with CHOP (censored at time of ASCT)3
Time (Months)
N at risk
OR
Dosing
ADCETRIS + CHP CHOP
100
Abbreviations
Consolidative SCT therapy did not affect the results of the secondary endpoint of PFS in patients with sALCL3
PFS (sALCL population; censored at the time of ASCT)3 • Multi-agent chemotherapy has been the standard first-line treatment for sALCL for decades, with CHOP, or variants of it, being the most popular regimen5,7
Study design
References
47 43
37 37
*Post-hoc analysis.
NICE
Background
Study design
Efficacy
Tolerability
Dosing
Summary
NICE
Background
Study design PFS
Efficacy OS
Tolerability
Dosing
Summary
ORR/CR
Three-step approach to objection handling 1
This three-step approach to objection handling will help you provide comprehensive answers to address questions from HCPs. Although it is important that you use this approach with all HCPs, there may be instances when you do not need to use all steps (e.g. skipping the probe if the question is obvious).
Probe: ● Question the HCP to gain a more detailed understanding of the underlying driver of the objection (use only if needed)
ACKNOWLEDGE
Please note that this objection handler is intended to help you provide the best possible responses to HCPs. Your sales skills and judgment will help you to adapt this approach for specific HCPs.
ALUNBRIG
3 Acknowledge: Let the HCP know you understand their question and consider it to be important
2
ANSWER
OBJECTION HANDLER
UNMET NEED
ALTA-1L
EFFICACY
TOLERABILITY
ANSWER
CLOSE
●
Confirm: Confirm the question has been addressed to the satisfaction of the HCP
●
●
Transition: Resume the call dialogue at the point at which the question was raised
●
●
Answer: ● Provide a response to the objection following the “acknowledge and probe” interaction. If applicable, utilise approved resources (e.g. ALUNBRIG iSell, leave pieces) as part of the answer
(brigatinib)
®
●
●
CONVENIENCE
QOL
SUMMARY
See ALK+ aNSCLC, Think Brain Metastases, Choose ALUNBRIG For both intracranial and extracranial efficacy1
❍
ALUNBRIG provided superior systemic and intracranial efficacy vs crizotinib1 ❍ Halved the risk of disease progression or death vs crizotinib in ITT population
(BIRC-assessed mPFS of 24.0 months with ALUNBRIG vs 11.0 months with crizotinib, HR=0.49; P<0.0001)1
❍ Two thirds reduction in risk of intracranial disease progression or death in
patients with any brain metastases at baseline (BIRC-assessed intracranial mPFS of 24.0 months with ALUNBRIG vs 5.6 months with crizotinib, HR= 0.31; P<0.0001)1
ALUNBRIG has a generally manageable tolerability profile1
REFS
?
MOA
❍ In the ALTA-1L study, the most common (>25%) AEs of any grade included
diarrhoea, increased blood CPK, cough, hypertension, nausea, and increased AST1
ALUNBRIG comes with a convenient dosing schedule2 ❍ The only licensed first-line treatment for ALK+ aNSCLC that has a single tableta,
once-daily dosing regimen2–5
PI
ALUNBRIG delivered a sustained and significantly longer duration of improvement in quality of life vs crizotinib1 ❍ Median duration of improvement in GHS/QOL not reached with ALUNBRIG
vs 12 months for crizotinib (HR=0.27; P<0.0001)1,6
When responding to objections, be sure to align with the key messaging presented in the ALUNBRIG iSell where appropriate
a In circumstances where dose is modified from the recommended dose, more than one tablet may need to be taken. Please refer to the SmPC for full dosing guidance.2
Medical Science Liaison referral: There may be occasions on which you cannot answer specific medical questions; for example, if it concerns offlabel use of ALUNBRIG, or other products in the Takeda Oncology pipeline. Such questions should be referred to Medical Information or, at the request of the HCP, can be referred directly to a Takeda Oncology Medical Science Liaison (MSL) ● There are also a number of situations in which a KAM may refer to an MSL aside from responses to specific objections. Refer to the MSL Ways of Working SOP for guidance: SOP-TUK-MI-607 V5.0 MSL Ways of Working combined ●
Aside from crizotinib, ALUNBRIG was not studied versus other ALK inhibitors.1 Because there are no head-to-head trials, we can’t compare directly to other ALK inhibitors. It is not clear if differences in outcomes are related to the study drug or differences in study design and patient populations The approval of ALUNBRIG in the first-line was based on the ALTA-1L study versus crizotinib in adult patients with ALK+ aNSCLC who had not previously received an ALK inhibitor1 At the time the trial was designed, crizotinib was the standard of care for first-line treatment2–4 ALUNBRIG provided superior systemic and intracranial efficacy vs crizotinib5 ❍ Halved the risk of disease progression or death vs crizotinib in ITT population (BIRC-assessed mPFS of 24.0 months with ALUNBRIG vs 11.0 months with crizotinib, HR=0.49; P<0.0001)5 ❍ Two thirds reduction in risk of intracranial disease progression or death in patients with any brain metastases at baseline (BIRCassessed intracranial mPFS of 24.0 months with ALUNBRIG vs 5.6 months with crizotinib, HR= 0.31; P<0.0001)5
●
●
CLOSE
Would you like to discuss the ALUNBRIG efficacy data in more detail? Now that we’ve talked a little about the efficacy of ALUNBRIG, let me provide you with additional information that may be helpful to you when making first-line treatment decisions for your patients with ALK+ aNSCLC
NB: There is a “?” tab in the iSell which can be used reactively to ensure the clinician understands alectinib trial design and headline results. This should not be used to make direct comparisons of the data set but to ensure the clinician is clear on details of the ALEX study.
References 1. ALUNBRIG Summary of Product Characteristics. 2. ClinicalTrials.gov. NCT02737501 Available at: clinicaltrials.gov/ct2/show/record/NCT02737501. Accessed November 2020. 3. Xalkori. Summary of opinion (post authorisation). Available at: www.ema.europa.eu/en/documents/ smop/chmp-post-authorisation-summary-positive-opinion-xalkori_en-0.pdf. Accessed November 2020. 4. Solomon BJ, et al. N Engl J Med 2014;371:2167–2177. 5. Camidge DR, et al. J Clin Oncol 2020;38:3592–3603.
Confidential and proprietary business information. For internal use only.
ALUNBRIG (brigatinib) | OBJECTION HANDLER | 5
Confidential and proprietary business information. For internal use only.
Confidential and proprietary business information. For internal use only.
ALUNBRIG (brigatinib) | OBJECTION HANDLER | 15
C-ANPROM/UKI/ALUN/0006 | Date of preparation November 2020
Patient PI
EFFICACY | TOLERABILITY | DOSING | SUMMARY | GLOSSARY
What serious side effects do I need to look out for?
Nurse
Click tabs to explore key ALUNBRIG data, prescribing information and adverse event reporting Use the arrows to work through the case studies
Tell your nurse or oncologist straight away if you experience signs relating to any of the following:
Alunbrig dosing Explore two real-life ALUNBRIG® (brigatinib) patient experiences alongside relevant efficacy and safety data
If patient does not have hepatic/renal impairment:1 ● The starting dose for Alunbrig is one 90 mg tablet once daily for the first seven days (blue part of
initiation pack), and then one 180 mg tablet once daily thereafter (green part of the initiation pack)
Read Tom’s case
Read Susan’s case
A 60-year-old chef who has ALK+ aNSCLC that has progressed with CNS involvement after front-line treatment with crizotinib and is experiencing neurological symptoms.
A 73-year-old retired journalist with osteoarthritis, osteoporosis and hypothyroidism and chronic musculoskeletal pain.
Explore Tom’s experience of ALUNBRIG and the relevant supporting clinical data.
If patient has severe hepatic impairment (Child-Pugh class C):1
If patient has severe renal impairment (eGFR < 30 mL/min):1
Due to your liver condition, you will start treatment on a 60 mg dose once daily for the first seven days, and then a 120 mg dose once daily thereafter if well tolerated.
Explore Susan’s experience of ALUNBRIG after progressing on frontline crizotinib for ALK+ aNSCLC.
ALUNBRIG is indicated as monotherapy for the treatment of adult patients with anaplastic lymphoma kinase (ALK)-positive advanced non-small cell lung cancer (aNSCLC) previously treated with crizotinib.1 These are not the patients’ real names.
● Your dose will be escalated in this way so we can monitor how you respond to Alunbrig at the
Signs of muscle damage
Lung problems
Signs of inflammation of the pancreas
Signs of liver problems
Slow heartbeat
Increased blood sugar
High blood pressure
start of treatment and look out for certain side effects that occur in some patients being treated with Alunbrig1 ● Depending on how you respond to Alunbrig you may need your dose adjusted; we will make this
References 1. ALUNBRIG Summary of Product Characteristics.
decision if we need to when we monitor your progress January 2019 UK/BRIG/1810/0029k
Not for further copying or distribution
Due to your kidney condition, you will start treatment on a 60 mg dose once daily for the first seven days, and then a 90 mg dose once daily thereafter if well tolerated.
Vision problems
1. Alunbrig Summary of Product Characteristics.
CLIENT
PROJECT
WORK TYPE
Takeda Oncology
Isell detail aid
• E-Marketing Designs
CLIENT
Tenovus 1
Singing For Health Student Task Sheets Sheet One
Correlation or causation? The Task • Imagine that you work for a sunscreen company whose research team has developed a new product. Your job is to design a trial for this new sunscreen and find out if it is more effective than the existing products. It has been established that the new product is safe, but not whether it is more effective. • Explain how you could use a randomised control trial to compare the new product with the existing leading brand. • Explain why this would be a better test than simply handing out some samples of the new product to a few friends and asking them in a week’s time how it went.
Fundraising for Tenovus Cancer Care
Schools Education Programme Singing for health Secondary School Resource
Key Stage 3 and Key Stage 4 Science
tenovuscancercare.org.uk
2
tenovuscancercare.org.uk
www.tenovuscancercare.org.uk
Singing For Health Student Task Sheets Sheet Two
Teachers’ Guide Singing for Health This resource is divided into FOUR SECTIONS
Correlation or causation? The Task This story appeared in the Mail Online:
• Setting the Scene • Introducing Singing for Health and the concept of Randomised Control Trials
Introducing singing for health and the idea of randomised control trials.
Setting the scene
• Getting Better or Feeling Better • Reflecting on the Research
• Read the story and discuss what it says. Agree on the key points. • Find out what Nobel prizes are awarded for. • Did the researchers find a correlation? Suggest what evidence they had for this. • Explain why this doesn’t automatically mean that consuming milk and milk products causes more of a country’s population to be awarded Nobel prizes?
• Why might there be a link? • What would need to be done to establish whether or not there was a link?
Each section varies in length and is presented in a way that is flexible and can be used in a variety of ways, depending upon lesson length, available time and other learning activities being deployed.
Objectives: •
To understand what microscopes are used for
•
To understand what cells are and that they are affected by cancer
•
To explore the idea of ‘well-being’
Introduction: Begin by asking pupils if they know what a microscope is and what it does. This could be supported by showing images of a microscope or, even better, display one. Ask pupils to suggest what they think could be studied through a microscope. We would then recommend asking pupils to identify a range of magnified images e.g.
• In fact, the authors of the research report warned that it shouldn’t be taken as being causative. Why do you think they said this? MOTH’S EYE (SLIDE 1)
1
tenovuscancercare.org.uk
Singing for Health
Singing for Health
SALT CRYSTALS (SLIDE 2)
5
HEAD OF A MOSQUITO (SLIDE 3)
4
Singing for Health
Developing the investigation
Singing for Health
Section Header Placeholder
Secondary Key Stage 3/4
Tenovus teaching materials for secondary
Supplementary powerpoint
• Three sources of evidence are being gathered Questionnaires. One of the areas of research is finding out whether people feel positive and good about themselves. Gathering their responses will be important. Breathing measurements. Although the starting point for this investigation is a sense of well-being, it seems reasonable to expect singing over a period of time to have some effect on the performance of the lungs. Testing biomarkers from analysis of saliva samples. Biomarkers include indicators such as mood states, stress hormones and immune function chemicals.
•
CLIENT
PROJECT
WORK TYPE
Tenovus
Various marketing materials
• • •
Editorial Layouts New Business Visualisations PowerPoint Presentations
Think about each of these sources of evidence and why it’s being gathered.
•
Is each source testing the same thing?
•
Would you expect positive responses on one of these to mean that the researchers should get positive responses on the others?
•
What do you think they will find out?
CLIENT
Tropicana For media use only
For media use only
The
Go dness of Juice: MEDIA INFOGRAPHIC
INTRODUCTION
5
Know 200 ml VITAMIN C
Only 30% of adults aged 19-64 and 10% of children aged 11-18 meet the ‘at least 5 a day’ recommendation for fruit and vegetables i
A 200ml serving of 100% pure orange
juice counts once toward your 5 a day
People who drink orange juice are
100% pure orange juice only contains sugars
that are naturally contained within the fruit from which it
DIET
providing energy to refuel the body after an overnight fast. Breakfast (breaking-the-fast) provides the brain and body with the energy it needs to function properly. Enjoying a glass of 100% pure orange juice with a wholegrain cereal such as porridge can make a great breakfast. The vitamin C in juice can help your body better absorb the iron naturally present in the oats as well as helping to maintain healthy skin and gums. In addition, oats are high in fibre. A glass of 100% pure orange juice also provides: potassium, folate, a range of phytochemicals which emerging research indicates can be beneficial to health, and counts towards 5 a day. What better way to start the day?
KEEPING THE IMMUNE SYSTEM
IN WORKING ORDER
which is the body’s natural defence. 100% pure orange juice is an excellent source of vitamin C which helps protect the body’s cells from damage from oxidative stress. It also contains folate which helps maintain a healthy immune system as well as being essential for cell growth and maintenance.
more likely to achieve at least 5 a dayii
an antioxidant nutrient which is important in maintaining a healthy immune system and helping the body absorb iron from plant foods
LTHY HEDA BALANCED
Breakfast is widely considered to be the most important meal of the day
Eating food and drink rich in vitamin C and folate can help maintain a healthy immune system
A 200ml serving (approximately one small glass) of orange juice is an excellent source of vitamin C –
SUGARS
is made
100%
A DAY
AN
juicy
WITH A
BREAKFAST
Staying healthy starts with what we eat and drink and 100% pure orange juice can play an important role in a healthy, balanced diet.
Did You
KICK
START YOUR DAY
The Government’s healthy eating advice, the Eatwell Plate, demonstrates that 100% fruit juice can be part of a healthy, varied and balanced diet
100% pure orange juice is one of the most nutrient rich fruit juices iii
JUICY TIPS
Healthy FOR A
DIET
Tip
1
Drink a glass of juice a day with a meal
Drinking a glass of orange juice with a meal based on plant foods such as veggies, beans, lentils, whole grain nuts and seeds, can help to increase the uptake of iron from these foods which is needed for healthy blood
Tip
and porridge make 2 aJuice great breakfast
A breakfast of porridge with a glass of 100% juice ticks many key dietary recommendations: wholegrain, fibre, vitamin C, 1 of your 5 a day and just enough beta glucan to help lower cholesterol
3
Make your own muesli
Tip For a different breakfast option, why not make your own muesli and soak it in juice to give your breakfast some zing in the morning!
4 Eat colourfully!
Tip The different colours of fruit and vegetables are derived from plant components such as carotenoids and flavonoids that have been linked with health benefits such as protection against cerebrovascular diseases (conditions that develop as a result of problems with the blood vessels inside the brain) iv
5 Eat a varied diet
Tip Eat a varied and balanced diet to ensure you get the full complement of vitamins and minerals your body needs
For media use only
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Tropicana
Print and digital marketing materials
• Editorial Layouts • Gifs • E-Marketing Designs
THE ROLE OF FRUIT JUICE IN THE DIET How Does 100% FRUIT JUICE Fit Within a Healthy Diet? Most nutritionists and dietitians agree that 100% fruit juice can be part of a varied, healthy and balanced diet. A minimum of 150ml of 100% orange juice counts towards 5 a day. Orange juice is an excellent source of vitamin C and a good source of folate and potassium, all of which have a role in maintaining a healthy body. › Results from the National Diet and Nutrition Survey (NDNS)1 showed that adult 100% fruit juice consumers had a lower body weight, body mass index (BMI) and waist circumference than non-consumers2 › Fruit juice consumption was also associated with improved dietary quality and a lower risk of micronutrient inadequacy and it did not displace whole fruit or vegetable intake2 » Similar results were observed in the US National Health and Nutrition Examination Survey (NHANES)3 » Overall dietary quality (assessed by the Healthy Eating Index-2005) was shown to be positively associated with 100% fruit juice consumption4 › Fruit juice consumers ate more fruit and vegetable portions than non-consumers with:2
› Fruit juice consumers were also less likely to have intakes below the lower reference nutrient intake for vitamins A and C, folate, Mg, Se and Fe and superior intakes of Vitamin C, folate, thiamin, niacin, Fe, Mg, K, Zn & Se2 » Data from NHANES also revealed that consumption of orange juice was higher in those with lower BMI and consumers had higher intakes of certain vitamins and minerals5 › A higher percentage of children who consume orange juice met the estimated average requirement for vitamins A and C, folate and Mg6
» Adults: 5.1 vs. 3.7 portions a day » Children: 3.5 vs. 2.5 portions a day
EMERGING RESEARCH
Fruit ON
JUICE
Phytochemicals and fruit juice • Fruits, vegetables and 100% juices are an important source of a wide range of phytochemicals such as polyphenols • Citrus fruits and juices are a rich source of flavanones, polyphenolic compounds which are members of the flavonoid family
Orange juice, hesperidin and cardiovascular disease • A study has shown that orange juice, which is naturally rich in hesperidin, and an isolated form of hesperidin are both able to induce the modification of the expression of genes related to positive cardiovascular health7 • These effects were significantly greater after orange juice consumption compared to consumption of hesperidin alone, suggesting a synergy between other components within the juice7 • Hesperidin may also be responsible for the beneficial effects on vascular function which were observed following 4 weeks of orange juice consumption7
An educational resource for health professionals | November 2014
Flavonoids and health • Research suggests that flavonoids may, in part, be responsible for the health benefits of fruits and vegetables8,9 • Studies have revealed improvements in risk factors associated with cardiovascular disease and dementia following consumption of flavonoid containing foods10.11,12 Orange juice and cognitive function • Research suggests that certain flavonoid rich food and drink may influence cognitive function10.11,12 • In one study, drinking 250ml of orange juice a day for 8 weeks improved executive function and memory13
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World Hepatitis Alliance (WHA)
ATEIFTAICSTS: HEOP W TH
Know it. Confront it.
KN
Know the main routes of transmission of hepatitis
HEPATITIS
B
C
1
UNPROTECTED
2
BLOOD TRANSFUSIONS
3
SHARING
NEEDLES
This is hepatitis...
4
MOTHER TO
World Hepatitis Day: 28 July www.worldhepatitisday.info
5
USING THE
6
SHARING
7
SHARING
?*
SEX
The clock is ticking. Act now to protect a new generation.
CHILD
TOILET
Know it. Confront it.
UTENSILS
Know it. Confront it.
TOOTHBRUSHES & RAZORS
What you can do
*
HEPATITIS
1
SEE A
2
GET
HEPATITIS
HEPATITIS
B
C
DOCTOR VACCINATED
Hepatitis does not discriminate. 500 million people are infected.
The risk of transmission of hepatitis C during unprotected sex is considered very low, especially if you are in a long-term, stable relationship. This risk may be higher among men who have sex with men or if blood is involved.
This is hepatitis... Know it. Confront it.
This is hepatitis... World Hepatitis Day: 28 July www.worldhepatitisday.info
www.worldhepatitisalliance.org
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World Hepatitis Alliance (WHA)
FreeStyle Libre marketing material
• New Business Visualisations • Infographics
The clock is ticking. Act now to protect a new generation.
This is hepatitis... World Hepatitis Day: 28 July www.worldhepatitisday.info
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World Health Organization (WHO) THE ROLE OF INFECTION PREVENTION AND CONTROL IN PREVENTING ANTIBIOTIC RESISTANCE IN HEALTH CARE
• On average, 1 in every 10 patients is affected by health care-associated infections (HAIs) • Antibiotic-resistant HAIs can double or more, the likelihood of death • Over 50% of surgical site infections can be resistant to antibiotics
Your exclusive invitation from the
World Health Organization
Effective infection prevention and control (IPC) and water, sanitation and hygiene (WASH) stops the spread of antibiotic-resistant organisms
IPC and WASH in health care protects patients and health workers from avoidable infections
The World Health Organization (WHO) antimicrobial resistance (AMR) team are delighted to offer you the opportunity to participate in an exclusive interview with [INSERT REGIONAL / GLOBAL AMR SPOKESPERSON].
The building blocks of IPC and WASH in health care facilities are: • effective hygiene practices, including hand hygiene • core components of IPC programmes • a clean, well-functioning environment and I equipment P W
A
Every infection prevented is an antibiotic treatment avoided • Play your role in controlling antibiotic resistance! • Ensure IPC programmes are in place and champion IPC practices
This year’s World Antibiotic Awareness Week (WAAW) will be held from 13–19 November. This year’s key theme will focus on the importance of seeking advice from a qualified healthcare professional before taking antibiotics.
S
H
This leads to: • less spread of antibiotic-resistant organisms • a reduced need for antibiotics
C
IPC saves millions of lives every year EXIT
RSVP to this invitation to secure your exclusive interview with an WHO expert. Click here for more information on this year’s WAAW campaign and supporting materials
Sources: World Health Organization. Infection prevention and control. Available at: http://www.who.int/infection-prevention/en/ World Health Organization. Water sanitation and hygiene. Available at: http://www.who.int/water_sanitation_health/en/ © World Health Organization 2017. Some rights reserved. This work is available under the CC BY-NC-SA 3.0 IGO licence.
The role of
MISUSING AND OVERUSING
INFECTION PREVENTION CONTROL (IPC)
ANTIBIOTICS Taking antibiotics when they are not needed accelerates emergence of antibiotic resistance,
one of the biggest threats to global health
Overuse of antibiotics can cause bacteria to become resistant,
meaning current treatments will no longer work
It is the bacteria itself
– not the person or the animal – that becomes resistant to antibiotics
When bacteria become resistant to antibiotics, infections which are normally minor, such as bronchitis, sinus and ear infections, or urinary tract infections, may become
much more dangerous and require treatment with drugs that may be more expensive and more toxic Antibiotic resistant infections can longer hospital affect anyone, stays, higher of any age, in any country medical costs and more deaths Antibiotic resistant infections can lead to
You can help reduce antibiotic resistance.
Always follow the advice of a qualified health care professional when taking antibiotics
to prevent the spread of antibiotic resistance in health care The emergence of antimicrobial resistance (AMR) can be likened to a forest fire: once it takes hold, it can spread swiftly, with dire consequences.
The spread of microorganisms, including those resistant to antibiotics, can be stopped with good infection prevention and control (IPC) practices including the use of safe water, sanitation and hygiene practices (WASH) in health facilities.
WHERE WILL YOUR
NEXT MOVE
Without adequate IPC, health care facilities can become dangerous breeding grounds for bacteria and endanger the patients they aim to help – as well as staff working there.
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World Health Organization (WHO)
Various marketing materials
• • •
Editorial Layouts Social Media Content New Business Visualisations
• Implementation of core components of successful IPC programmes • Good hygiene practices and precautions • Clean environment • Safe water • Adequate sanitation
Good IPC practices may reduce transmission of infections in health care facilities by half, saving millions of lives every year.
The emergence and spread of antimicrobial resistance (AMR) are largely due to the inappropriate use of antibiotics and poor IPC practices.
On average, 1 in every 10 patients is affected by HAIs worldwide1 and improved IPC practices can lead to more than a 30% reduction in HAI rates.
Healthcare-associated infections (HAI) can prolong hospital stays and create long-term disability – when resistant to antibiotics, can double the risk of death.
The spread of AMR is similar to that of a forest fire, with effective antibiotics representing the fire fighters needed to put out the fire – reducing AMR. However, in many cases these effective antibiotics are still at least 5 years away in their development and in the meantime, good IPC practices can be used as a ‘fire break’ to stop the spread of AMR.
Every infection prevented is an antibiotic treatment avoided – effective IPC is critical to tackling AMR. • Be a champion of IPC practices and play your role in controlling the spread of AMR. • Be a leader to ensure the core components of effective IPC programmes are in place in your facility.
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IPC helps to control the spread of infection within health care facilities and consists of:
Effective IPC practices are critical to tackling the emergence and spread of AMR, by: • reducing the need for antibiotics by reducing the risk, transmission and spread of infections that require the use of antibiotics • reducing the spread of already circulating resistant pathogens
TAKE YOU?
Find out more about Mobility via http://intranet.who.int/sites/mobility/, or contact Human Resources at: globalmobility@who.int.
IPC is a practical, evidence-based approach preventing patients and healthcare workers from being harmed by avoidable infections.1
• PowerPoint Presentations • Infographics
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World Health Organization INTRODUCING
GEO MOBILITY:
Country
Headqu a
rs rte
LAUNCH OF THE VOLUNTARY PHASE
Reg i
al on
VECTOR
BORNE
DISEASE
MAJOR
COPENHAGEN DENMARK
GENEVA
SWITZERLAND
OFFICES IN
Geographic (Geo) Mobility i Move for health
CAIRO
MOBILITY
EGYPT
NEW DELHI INDIA
MANILA
PHILIPPINES
BRAZZAVILLE CONGO
Geographic Mobility is an opportunity for WHO staff members to rotate to positions globally to help address the increasingly complex public health challenges of the 21st century.
A VECTOR TRANSMITS A DISEASE FROM
ONE HOST TO ANOTHER
Geo Mobility strengthens the power of ‘One WHO’ with stronger working relationships and greater knowledge sharing across the Organization. Geo Mobility will further upskill the existing, workforce to be increasingly dynamic and adaptable.
Some vector-borne diseases have been around for over
Account for around
Seeking a new challenge? Move to expand your personal and professional
Mobility i Move for Health
17%
i
of infectious disease cases
400 YEARS
Mobility is an opportunity for WHO staff members to rotate to positions globally to help address the increasingly complex public health challenges of the 21st century. Mobility strengthens the power of ‘One WHO’ with stronger working relationships and greater knowledge sharing across the Organization. Mobility will further upskill the existing workforce to be
horizons
Key Mobility Facts
people travelled outside their native country last yearii
and experience by working in a variety of duty stations across the Organization.
Experience different countries and cultures, learn from and transfer knowledge to other WHO colleagues and further build your career within the Organization.
Seize the opportunity: Choose your move
VECTORS
can be microscopic, but in some cases deadly
HIGH RISK AREA
THE USUAL SUSPECTS
Embrace Mobility: Move with your family
The first compendium includes a variety of technical and
Around
You are at risk if you visit or inhabit a
During the voluntary phase, the opportunity is open to WHO staff members on a fixed-term and continuing appointment, irrespective of the number of years already served in the current duty station. For more information and eligibility criteria go to (http://intranet.who.int/sites/mobility/), or contact Human Resources at: globalmobility@who.int.
increasingly dynamic and adaptable.
1 BILLION
Geo Mobility represents an exciting personal and professional development opportunity for staff to broaden their skills, knowledge
of WHO staff are eligible to take part in Mobility in the voluntary phase
management roles
geographically spread across
the three levels of the Organization
Mobility will cover
150+ country offices 5 regional offices and headquarters
3 years for voluntary phase, 3 weeks to apply once the Mobility compendium is published,
can apply for
3 positions
Where can I get more information?
This tiny mosquito…
http://intranet.who.int/sites/mobility or by email at:
Malaria
WHO is committed to supporting and ensuring a smooth transition for colleagues and their families when moving to a new post as part of the Geo Mobility programme.
May carry , which affects 275iii million people each year, killing 1.2iv million of them or even
typhus
leishmaniasis, which eats at the skin
Your next move
dengue fever
The first Mobility compendium (http://intranet.who.int/sites/mobility/) contains the list of open Eligible staff can apply for up to three positions. The deadline will be specified for three weeks after the compendium is published. If your application for Geo Mobility is successful you will be contacted by HRD by the end of March.
Bats carry the
hendra virus,
Up to 100 million cases of
and even
are reported annuallyv
posts.
globalmobility@who.int
The tiniest of fleas can transmit
rabies
Move to grow personally and professionally Mobility represents an exciting personal and professional development opportunity for staff to broaden their skills, knowledge
and experience by working in a variety of duty stations across the Organization. Experience different countries and cultures, learn from and exchange knowledge with other WHO colleagues and further build your career within the Organization. Experience at the 3 levels of the Organization will position you better for future advancement opportunities.
Key Geo facts The first compendium will include a variety of
technical and management roles geographically spread across the three levels of the Organization
Around of WHO staff are eligible to take part in Geo Mobility in the voluntary phase
Embrace Mobility: Move with your family
Geo Mobility will cover
3 years for voluntary phase, 3 weeks to apply once Mobility
compendium is published, can make up to
3 choices
157+ country offices 5 regional offices and headquarters
WHO is committed to supporting and ensuring a smooth transition for colleagues and their families when moving to a new post as part of the Mobility scheme.
Seize the opportunity: Choose your move
Geographic Mobility will be gradually rolled out across the Organization over the next three years on a voluntary basis, becoming mandatory in 2019 End of January first voluntary compendium issued
YOU CAN
The deadline will be specified for three weeks after the compendium is published End of March, applicants notified of the outcome of their application Successful colleagues will usually be asked to move to their new position within three months
REDUCE YOUR CHANCE
During the voluntary phase, the opportunity is open to WHO staff members on a fixed-term and continuing appointment, irrespective of the number of years already served in their current duty station.
OF CONTRACTING ALL OF THESE CONDITIONS
COPENHAGEN
REGIONAL
OFFICES
DENMARK
CAIRO
NEW DELHI
EGYPT
INDIA
Timeline
MANILA
PHILIPPINES
BRAZZAVILLE CONGO
Mosquito nets, insect repellents, antimalarial tablets and vaccinations
Long-sleeves can protect the skin
Take extra precaution when working near irrigated water systems
Where can I get more information? http://intranet.who.int/sites/mobility or by email at: globalmobility@who.int
Geo Mobility will be gradually rolled out across the Organization over the next three years on a voluntary basis, becoming mandatory in 2019. Geo Mobility will be evaluated annually during the voluntary phase with feedback from staff members, supervisors and staff representatives, to improve the policy and process in following years.
References i WHO ‘Exploiting the potential of vector control for disease prevention’ who.int/bulletin/volumes/83/12/942.pdf [August 2013] ii Reuters ‘International tourism to reach record 1 billion travellers in 2012’ in.reuters.com/article/2012/12/06/tourism-record-idINDEE8B50GK20121206 [August 2013] iii WHO ‘Six diseases cause 90% of infectious disease deaths’ who.int/infectious-disease-report/pages/ch2text.html [August 2013] iv WHO ‘Vector-borne disease’ who.int/heli/risks/vectors/vector/en/ [August 2013] v WHO ‘Dengue and severe dengue’ who.int/mediacentre/factsheets/fs117/en/ [August 2013]
The voluntary phase of Geo Mobility is a new opportunity for personal and professional development and one which will offer equal benefits to the Organization.
Mobility will be gradually rolled out across the Organization over the next three years on a voluntary basis, becoming mandatory in 2019
End of January 2016 first voluntary compendium issued
PROJECT
WORK TYPE
World Health Organization (WHO)
Various marketing materials
• • •
Editorial Layouts Social Media Content New Business Visualisations
End of March, applicants notified of the outcome of their application
Successful colleagues will usually be asked to move to their new position within three months
Where can I get more information?
http://intranet.who.int/sites/mobility or by email at:
globalmobility@who.int
Job number: XXXXXXXXX Date of prep: August 2013
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The deadline to apply is three weeks after the compendium is published
• PowerPoint Presentations • Infographics
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Avanos BRAND GUIDELINES
Released July 2018 Version 1.0
CORTRAK* NJ FEEDING
REDUCING RISK REDUCING COST
CORTRAK*: PROVIDING SOLUTIONS TO CHALLENGES
CORTRAK* is FDA cleared and studies have shown that CORTRAK* can confirm feeding tube placement at bedside without x-ray1–3
REDUCING RISK, REDUCING COST FOR NJ FEEDING IN ADULTS
2-4%
66%
EARLY ENTERAL NUTRITION IS ESSENTIAL TO AVOID THE CONSEQUENCES OF MALNUTRITION
5x
Greater likelihood of DYING5
15.5 MINS
Greater likelihood of DEVELOPING SURGICAL SITE INFECTIONS4,6,7
An estimated 1/3 of patients enter hospital malnourished4
4x
1.5x
Greater risk of REMISSION within 15 DAYS8
Greater likelihood of DEVELOPING PRESSURE ULCERS4,6,7
NJ, nasojejunal.
WITH CORTRAK*, EVEN PATIENTS WITH DGE CAN RECEIVE MORE EFFECTIVE NUTRITION COMPARED TO USING PROKINETICS ALONE5 † Based on a systemic literature review of nine studies.
6. Barker LA, et al. Int J Environ Res Public Health 2011;8(2):514–27
1. Gray R, et al. Nutrition Clin Pract 2007;22(4):436–44
7. Guenter P, et al. J Qual Patient Safety 2015;41(10):469–73
2. Smithard D, et al. Dysphagia 2015;30:275–285
8. Lim SL, et al. Clin Nutrit 2012;31(3):345–50
3. Taylor SJ, et al. Br J Intensive Care 2010;(summer):38–44 4. Nguyen N, et al. Crit Care 2007;11(1):R16 5. Taylor J, et al. J Parenter Enteral Nutr 2010;34:289–294 6. Koopmann MC, et al. Ann Surg 2011;253(2):297–302 7. Taylor SJ, et al. Intensive Crit Care Nurs 2019;55:10276629
aspHirate pH INDICATOR STRIPS INNOVATING THE STANDARD – HOW TO USE GUIDE
4.0
4.5
5.0
5.5 3 4.5
6.0
4
6.5
7.0 5 min
pH• Indicator strips for the colour change to complete Wait for 30 seconds
For •professional use only The strip can be read
IVD
≥ 7.5
15°C
Implementation of an electromagnetic imaging system to facilitate nasogastric and post-pyloric feeding tube placement in patients with and without critical illness
for up to 5 minutes, discard after use
2
150.1 1500001 04-2022
patients included in analysis
referrals for post-pyloric feeding
had tubes successfully fit
referrals for nasogastric feeding
had tubes successfully fit
22%
£111
0%
£120
request for X-ray confirmation on post-pyloric placements
request for X-ray confirmation on post-pyloric placements
Mean cost per tube insertion
Mean cost per tube insertion
CORTRAK* confers clinical and cost advantages in the real-world setting
Authorised Representative
Distributor
Johnson Test Papers Ltd Hainge Park, Hainge Road Oldbury, B69 2NU United Kingdom
Avanos Medical Belgium BVBA Leonardo Da Vincilaan 1 1930 Zaventem Belgium
Tel: +44 (0)121 557 3883 Email: cs@jtp.uk.com
Tel: +00 000 000 0000 Email: avanos@avanos.com
INTRODUCTION
METHODS
Blind placement of feeding tubes at the bedside can be problematic and may require x-ray confirmation if pH testing of tube position is inconclusive. Endoscopic guidance may be used but presents challenges in terms of staffing and costs. Alternately, parenteral nutrition may be considered, however this method has numerous potential clinical considerations and is generally more costly.
A retrospective analysis of the CORTRAK* system database and medical, dietetic and nursing records was undertaken across 14 months (October 2007 to December 2008) at Pinderfields General Hospital (hospital A) and Dewsbury and District Hospital (hospital B) within Mid Yorkshire Hospitals NHS Trust. Data were collected on:
Electromagnetic sensing devices (ESD) can be used to facilitate bedside placement of nasogastric and post-pyloric feeding tubes. This study aimed to audit referral trends, practice and effectiveness of placement of nasogastric and post-pyloric feeding tubes after implementation of an ESD tube placement system (CORTRAK*) within Mid Yorkshire Hospitals NHS Trust.
Registered Trademark or Trademark of Avanos Medical, Inc., or its affiliates. ©2019 AVNS. All rights reserved. HC988-00-UK
• The origin of patient referral (clinical speciality and referral source) • Reasons for CORTRAK* placement • Nutritional status and preparation of the patient • Duration of placement procedure • Successful placement rates • X-ray confirmation requests due to inconclusive final images
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Print marketing materials
• Editorial Layouts • E-Marketing Designs • PowerPoint Presentations
ENSURING ACCURATE PLACEMENT
Success rate for post-pyloric placement in children for CORTRAK* vs 39.0–76.3% for blind placement1–3
Significantly fewer abdominal x-rays required to check placement (0.6–1.3 for CORTRAK* vs 1.63–2.4 for blind placement)1,2
1. NICE. Medtech Innovation briefing. Available from: www.nice.org.uk/advice/mib48/resources/cortrak-2-enteral-access-system-for-placing-nasoenteral-feeding-tubes-pdf-63499172779717. Last accessed August 2020; 2. Goggans M, et al. Nutr Clin Pract 2017;32(2):233–7; 3. Prashant J, et al. Crit Care Med 2019;47(1):211.
CORTRAK* NJ FEEDING
REDUCING RISK, REDUCING COST FOR NJ FEEDING IN CHILDREN GETTING IT RIGHT FIRST TIME
Journal of Human Nutrition and Dietetics 2010;23:61–68
Retrospective review of CORTRAK* use across first 14 months at two hospitals
36 29 20 7 3
container
• Document as per25°C local policy
LOT
5.5
5.0 5.5
aspHirate
6.0
5.0
4.5
6.0
• Place 2 –3 drops of the aspirate from the syringe on the each pad of the indicator strip o Ensure each pad is completely wetted, allowing excess aspirate to run off the indicator strip onto an absorbent towel
pH test strips for the semi-quantitative • Compare the colours on tube the indicator strip with the scale on the indication of pH in human gastric aspirate for the assessment of correct the tubestrip has been removed from o Always use the container placement.
1.5–1.7 HOURS Time to successful post-pyloric placement in children for CORTRAK* vs 4.6–21.0 hours for blind placement1,2 • A study with experienced paediatric nurses reported time to placement of 3 mins vs 20 mins for CORTRAK* vs blindplacement3
82.0– 100% CORTRAK* virtually eliminates the risk of tube misplacement (0% vs. 1.77% misplacements with conventional methods)†,2 • However, tube misplacements can occur if healthcare professionals are not suitably trained7
Windle EM, et al.
≤ 3.5
2 30 sec
CORTRAK* allows visualisation at bedside and immediate identification of misplaced tubes to minimise the risk of complications, such as lung placements1,6
PUBLICATION DISCUSSION GUIDE
Method for testing
2 - 3 drops
Delayed gastric emptying (DGE) occurs in up to 60–70% of intensive care patients and can prevent adequate enteral nutrition3,4
2. Smithard D, et al. Dysphagia 2015;30:275–85
5. Corkins MR, et al. J Parenteral Enteral Nutr 2014;38(2):186–95
Method for testing
Studies suggest that inadvertent placement into the bronchi occurs in 2–4% of blind placements2 • Equates to 5,000–110,000 misplaced tubes per annum in the UK, with the potential to cause significant morbidity and mortality2
Average time to placement of post-pyloric tubes for CORTRAK* vs 42 mins for blind placement†,2
3. FDA. Feeding tube placement systems. Available from: https://www.fda. gov/medical-devices/letters-health-care-providers/feeding-tube-placement-systems-letter-health-care-providers. Last accessed August 2020 4. Tappenden KA, et al. J Acad Nutrition Dietetics 2013;113(9):1219–37
1
Reduction in the time between order for tube placement and initiation of feeding1
2x
60-70%
1. Windle E, et al. J Hum Nutr Diet 2010;23:61–8
CORTRAK*: PROVIDING SOLUTIONS TO CHALLENGES PROVIDING TIMELY FEEDING
PROVIDING TIMELY FEEDING
GETTING IT RIGHT FIRST TIME
An additional 1/3 will develop malnutrition during their stay4
ENSURING ACCURATE PLACEMENT
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Nature’s Creations Ltd
Huna product launch
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We’re meticulous when it comes to producing CBD. Our hemp experts oversee every stage of the process bringing you pure unadulterated Huna. Whether you’re looking for
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connect you with the awe-inspiring power of nature.
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CooperVision Getting started with myopia management in practice
Managing myopia matters
uccessfully 8 and
What can we do?
In the UK, the number of children aged 10-16 with myopia has more than doubled over the last 50 years. Today, children are becoming myopic at a younger age meaning that they are more likely to progress faster and have higher levels of myopia.1
ws both axial length
Everyone with myopia has potential for significant ocular health risk, including increased risk of:2
Incidence of myopia in 10—16 year olds has more than doubled in the UK in the past 50 years1
⦿ Retinal detachment
Slowing progression of myopia by one dioptre in children can lower risk of myopic maculopathy by 40%3
Everyone with myopia has potential for significant ocular health risk2
⦿ Myopic maculopathy
1. Assess the risk for myopia
Myopia is a significant and increasing public health issue
• Children with myopic parents are more likely to become myopic themselves5 • Age six is a key milestone for predicting risk: +0.75D or less of hyperopia may suggest a myopic future, regardless of family history6
By 2050, 50% of the global population will develop myopia1
50%
2. Behavioural management
⦿ Glaucoma
• Spending time outdoors is protective for myopia development, but the mechanism is poorly understood7
⦿ Cataracts
• A minimum of 10 hours per week outdoors is an achievable recommendation7
Risk of myopia: How to raise parental awareness A YouGov survey commissioned by CooperVision identified that parents:4*
10
In Western Europe, 56% of the population are predicted to be myopic by 20501
56%
hrs
Myopia increases the risk of serious, sight-threatening eye diseases, such as:2
3. Getting started • Start building experience fitting young children with contact lenses and have your practice environment set up appropriately
Myopic maculopathy
• Adapt your approach to exams and ensure staff are well trained, especially for teach appointments
Retinal detachment
Glaucoma
Cataracts
• Provide parent and child friendly resources Are mostly unaware that the progression of myopia can be slowed
Are unaware of the health risks associated with myopia
Believe that eye care professionals should provide them with information about all options for myopia management
Parents are twice as likely to consider contact lenses for their child if recommended by an ECP
2
X
• Be friendly and use positive body language
Together we can help change the future ofchildhood myopia
• Take a look at the MiSight® 1 day website at coopervision.co.uk/contact-lenses/ misight-1-day
Introducing MiSight® 1 day daily disposable contact lenses, proven to slow the progression of childhood myopia. In a clinical study over three years, MiSight® 1 day demonstrated:3
4. Consider MiSight® 1 day MiSight® 1 day is the first daily disposable contact lens proven to slow the progression of myopia in children8*
In a robust, randomised controlled clinical study, currently in its seventh year and published in a peer-reviewed journal, MiSight® 1 day reduced the rate of myopia progression by 59% and reduced axial elongation by 52%8*
2-60. 3. Bulliomore M & 7–31. 5. McCullough S 1): 115–121. 7. Gifford lline J, Jones L, Sinnott
59%
52%
41%
reduction in myopia progression
reduction in axial elongation
showed no meaningful progression in refractive error vs. 4% using standard single-vision one-day lenses
ts subsidiaries. *The online survey selected 280 British adults. The survey included questions concerning the opinions of parents regarding contact lenses, the role of ECPs, their feelings about their child’s diagnosis, their attitudes towards their child wearing contact lenses (given different scenarios), and their understanding of myopia and its management.4
*Compared with a single-vision, one-day lens over a three-year period in children aged 8–15 years on a recommended minimum wearing time: 6+ days per week, 10+ hours per day.
THE PATIENT JOURNEY
Consider growth of the eye and the increased risk this poses to visual impairment. Drag the line to show the risk of visual impairment associated with axial elongation.
Click on each step in the patient journey to review the key actions and the support tools on offer. APPOINTMENT
<26mm:
0%
ACTIONS
100% 3.8% risk of visual impairment
..................................................................
RECAP OF VISUAL IMPAIRMENT AND AXIAL LENGTH
Comprehensive eye exam • Symptoms and history • Habitual visual acuity (distance and near) • Autorefraction and keratometry • Manifest refraction (cyclo recommended) • Best corrected visual acuity (distance and near) • Binocular status • Ocular health • Document myopia management advice given based on findings and risk assessment guide • Demonstrate myopia with Vision Simulator • Provide Guide to Myopia Management to parents
START
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20
30
40 PREVIOUS
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• Vision simulator • Parent/Patient Guide to Myopia Management • Risk Assessment Guide • Axial length estimator (advanced support) • Centile-based eye growth and refractive error charts (advanced support)
Ensure glasses condition is checked and records kept at all appointments
“MiSight 1 day contact lenses can provide long-term benefits to your child’s sight – it is important to slow short-sightedness progression early! ®
How to manag e child’s screen your time during lockdown: 1. Take a bre ak from online learning and use books or other printed resources 2. Set aside times to unp lug and write by hand 3. Keep active throughout the day 4. Spend tim e outdoors 5. Stop usin g digital dev ices at least an hou r before bed
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Indie Grewal Optometrist and President of the British Contact Lens Association
Look familiar? With Coopervision, kids can enjoy the benefits of spectacle free vision
Don’t let your child’s prescription limit their ambition”
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MiSight® 1 day reduces short-sightedness progression in children by
59% on average
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European Migraine & Headache Alliance (EMHA)
I AMMORE THAN MY MIGRAINE
#morethanmymigraine
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European Migraine & Headache Alliance (EMHA)
Various marketing materials
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Swedish Orphan Biovitrum (Sobi) Introduction & tips
PAIN IN HAEMOPHILIA What is pain?
A new partner
my voice: talking with others about haemophilia
my voice, my care
Pain is the body’s way of saying something isn’t quite right – a warning sign that damage is occurring or about to happen.1,2 1,2
for people living with haemophilia
Many people with haemophilia have their own personal experience of pain.11However, it should not be considered the ‘norm’. Pain can be managed and prevented.1
Your partner’s family New friends and peers
le pouvoir du jeu
Types of pain Pain in haemophilia is often related to bleeding into joints. There are two types – although hard at times, it’s important to tell them apart as they are managed differently.1
Acute pain
Chronic pain
• Sudden short-term pain, lasting hours or days
• Persistent longerterm pain, lasting months or longer
• May feel like throbbing, sharp pain or tenderness
• May feel like aching, stiffness or ongoing discomfort
1,3–5
People at work
A guide to talking with your healthcare team about what you want to achieve and what you want your treatment and care to do for you.
Pain sites
Ce guide est conçu pour aider votre enfant à mener une vie saine et heureuse grâce à l'activité physique
Pain can occur where bleeds happen.1 The most common bleeding sites in haemophilia are the hinge joints (ankles, knees and elbows).6
1,3–5
HOW CAN PAIN BE MANAGED? Healthcare professionals
1•
As they have different causes, acute and chronic pain are managed differently. There are medical and non-medical approaches to help treat both types.1
Acute pain
Chronic pain R.I.C.E method
Relaxation techniques4
(within 24 to 48 hours)4,5,7,8 Protects from further injury and helps reduce bleeding and swelling.
Help reduce tension and stress.
Prompt treatment1,8 Acute pain caused by a bleed* typically lessens after treatment with clotting factor therapy.
Surgery 1,9,10
*Pain can also occur without a bleed.
Top tips to help take control of your haemophilia
To restore or correct the affected joint.
Working and Travelling around the World with Haemophilia
Both pain types
May 7, 2020
May 7, 2020
As people who live with haemophilia every day, we bring a unique level of expertise and knowledge that can, and should, shape the healthcare that we receive. We live in a time when modern healthcare systems are trying to move towards more personalised and patient-centred forms of medicine, with aims to empower people to have more of a say in all of the aspects that affect their health. The European Patients Forum describes patient empowerment as enabling patients “to be involved in the decision-making and management of their condition according to their preference.”
Growing up, I was often worried about how my haemophilia might impact my ability to travel the world… with bulky boxes of Factor 8, vials that needed to be kept in a fridge, never mind thinking about needles and airport security! My first experience of travelling abroad with haemophilia came whilst I was at university. As part of my studies, I had the opportunity to apply for an Erasmus+ placement in Slovakia, to work on, and learn from, a project developing nature conservation and eco-tourism. It was quite a leap to go from never having been out of the country before to travelling on my own to live and work in a new country for 6 weeks!
But what does this actually mean for us as people with haemophilia? What can you do to become empowered? Here’s some of my experiences…
Protection from bleeds1,8
Be informed One of the greatest ways that I’ve found to be empowered to have more control over my health and haemophilia is to learn more about it – this has been called ‘health literacy’. It might seem slightly contradictory that I’m suggesting that ‘living life beyond haemophilia’ involves engaging with it more. However, from my own experience, I’ve found that having the knowledge, understanding and confidence to ask relevant questions during meetings with clinicians can be crucial to becoming an active partner in decision-making processes and accessing the kind of treatment that I want. Challenging the status quo of today’s haemophilia care is about being able to ask for what you want and knowing what this might be. We’re lucky to live at a time when the accessibility of information is greater than ever before, and have routes to learn about our treatment options from a wide range of sources. The World Federation of Haemophilia is a great place to start, for example.
Be part of the haemophilia community Following on from this, we’re also living in a time when it’s easier than ever to connect with other people with (or affected by) haemophilia. As someone with no family history of haemophilia, no siblings with haemophilia, and having attended small clinics my whole life, it’s rare that I’ve had a chance to discuss my experiences with others. However, with the internet, whole communities of people living with haemophilia have formed, allowing us to explore topics of concern together, empowering one another through sharing similar stories and questions. Online platforms and haemophilia patient forums (e.g. Reddit) are a fantastic source of advice, solidarity, and current developments. Similarly, there is also a thriving community of people with haemophilia on Twitter. The main challenges here are whether to search for an Americanised or anglicised spelling! Being part of these communities have shaped my experiences of my own haemophilia and my sense of wellbeing in knowing I’m not alone. It’s also given me access to learn from, and discuss haemophilia, with a range of different people – including other people with haemophilia, of different ages and geographic contexts, clinicians with different perspectives and expertise, and researchers at the cutting edge of haemophilia. It’s meant having my own preconceptions about haemophilia challenged, learning and being inspired by the achievements of others. Doing this empowers me to have greater control over the decisions and actions affecting my haemophilia, and enables me to be confident that I can live my life beyond haemophilia.
Pain relievers5,8
Physical therapy 4,8,11
Over-the-counter or prescription pain relief medicines may be appropriate.
Future bleeds can be prevented with prophylactic therapy.
Helps manage pain and restore joint function.
Building a nature trail through wetland forest in Slovakia
Calculating the right amount of treatment to take was a challenge, and looking back, I’m not sure I got my maths right! Towards the end of the 6th week, I was running very short on treatment. It was certainly a learning experience though, and has taught me valuable lessons about always overestimating the amount of treatment I need, factoring in for bleeds, and even taking extra needles for when an initial attempt to find a vein goes wrong. The Haemophilia Society in the UK recommends taking ‘2-3 times the amount of factor you normally need’ when travelling – though for long trips, this can quickly take up a huge amount of space in your luggage. Particularly when the advice is often to stash treatment in your hand luggage, so that it doesn’t get lost or damaged in the hold.
COPING WITH PAIN
Since then, I’ve been lucky enough to travel around the world, though am always much more careful to have extra treatment with me after my initial close-call! My earlier anxieties about being stopped at security have never actually been realised – in fact, my iPad has caused me more trouble at security than my medication ever has! Though, following the World Federation of Haemophilia’s tips of travellers, I always make sure I have a letter from my clinicians to explain why I’m carrying treatment – just in case.
Pain is not just a physical discomfort, it’s also an emotional experience1,2 that can have an impact on:
Be involved in research The role played by people with haemophilia in research is changing. Scientific and healthcare researchers are increasingly keen to actively involve patients in research, doing research ‘with’ people affected by the research, rather than ‘to’, ‘about’ or ‘for’ them. Whilst haemophilia doesn’t have the same culture of involvement as other health conditions, this is growing, and will be a vital part of the future of haemophilia. Seizing these new opportunities and being involved in research allows us, as people with haemophilia, to set the agenda, and have a say on the kinds of questions that we think are important priorities and should be addressed. Examples include, The Bleeding Disorders Priority Setting Partnership, where people with haemophilia contributed to producing a list of the most pressing questions for our community, as defined by us. The People in Research website, along with The Haemophilia Society’s research page, are good places to keep an eye on for opportunities to be empowered to shape the future of haemophilia research, treatment, and care.
Estonia and Arizona – two places that my work has taken me to – something that, when I was younger, I would never have dreamed would be possible with my haemophilia.
Since then, I’ve been lucky enough to travel around the world, though am always much more careful to have extra treatment with me after my initial close-call! My earlier anxieties about being stopped at security have never actually been realised – in fact, my iPad has caused me more trouble at security than my medication ever has! Though, following the World Federation of Haemophilia’s tips of travellers, I always make sure I have a letter from my clinicians to explain why I’m carrying treatment – just in case.
James Gorman
James Gorman
30, severe haemophilia A
30, severe haemophilia A
Daily life12
Connecting with others12,13
Being less able to carry out everyday tasks.
Wanting to socialise less with others. Having a low mood (feeling irritable, tense or withdrawn) that impacts relationships.
Personal growth12,13 Enjoying yourself 12
Feeling less productive and needing to take time off work or study.
Being less involved in usual leisure activities.
There are ways to help you cope.
STAYING ON TOP OF MENTAL HEALTH Everyone experiences and copes with pain differently.1 Pain can lead to negative emotions,5,13 which in turn can cause pain to feel worse.1,14 Below are some tips that could help you keep on top of things.
October, 2020 October, 2020
Thought Leaders: Adhering to exercise plan during the COVID-19 pandemic
Thought Leaders: Adhering to exercise plan during the COVID-19 pandemic
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1 1 Quality of life
Physical activity and treatment adherence during Covid-19 and the need to continue to do so
Engage in low-intensity exercise4,11,14 Easing into a routine that suits you can help improve mood, mobility and pain.
“
Find a way to relax and reduce tension4,14
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Quality of life Physical activity and treatment adherence during Covid-19 and the need to continue to do so
READ MORE
SELF-HELP & WAYS TO TAKE CHARGE
Sleep well14,15 A good night’s sleep boosts mood. If you struggle to sleep because of pain, ask your healthcare team for support.
Meditating or breathing exercises won’t necessarily make the pain go away but may help you cope.
”
Stay in control1,13 Unhealthy behaviours to help cope with pain (for example, becoming dependent on substances) can lead to other health issues. If you relate to this, speak with your doctor as soon as possible.
Leadership Articles
Leadership Articles DOWNLOAD
DOWNLOAD
Get your team involved
2 The future of Haemophilia care post Covid-19:
You should not feel like you have to ‘put up’ with pain or face it alone. Try to open up with your haemophilia care team about how you are feeling. They can help provide psychological support and may prescribe medicine to help.8,13,16
2
Case studies
The future of Haemophilia care post Covid-19:
VIEW
technologies, ways of working, how Sobi can support the community
technologies, ways of working, how Sobi can support the community
If you would like to learn more about how to live well with haemophilia, you can explore information, advice and stories at www.LiberateLife.eu <local markets to update with relevant URL>. Any medical information is for informational purposes only and is not a replacement for advice given by a physician or other medical professionals.
REFERENCES Sobi is a trademark of Swedish Orphan Biovitrum AB (publ) © 2020 Swedish Orphan Biovitrum AB (publ) – All rights reserved Swedish Orphan Biovitrum AB (publ) SE-112 76 Stockholm, Sweden, +46(0)8 697 20 00 NP-9769 | Date of preparation: March 2020
Physical activity and treatment adherence during Covid-19 and the need to continue to do so
Video Media
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Swedish Orphan Biovitrum (Sobi)
Print and digital marketing materials
Understanding the post-Covid patient:
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keeping up health during COVID, connecting with others and resources available on the Sobi website (LiberateLife.eu) to help communities and care teams keep in touch
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3 Understanding the post-Covid patient: keeping up health during COVID, connecting with others and resources available on the Sobi website (LiberateLife.eu) to help communities and care teams keep in touch
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
• E-Marketing Designs • Website Design • Infographics
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Siemens
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Siemens
Financial Services Brochure Mastercard Booklet
Print Design Marketing Collateral
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SAS - Scandinavian Airlines
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Scandinavian Airlines (SAS)
Scandinavian Airlines in China
Brand localization Magazine Advertisements Online Marketing
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SAS - Scandinavian Airlines
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Scandinavian Airlines (SAS)
Beijing-Stockholm Direct Flights
Brand localization Magazine Advertisements Marketing Material Event Management
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The Association of MBAs
IS THE GOOD OF SOCIETY INTEGRAL TO GOOD BUSINESS? BRIGHT MINDS WANTED TO SHAPE THE FUTURE OF MANAGEMENT
MBA STUDENT OF THE YEAR
AWARD 2012 NOMINATIONS NOW OPEN. ASK YOUR SCHOOL FOR DETAILS
Our previous MBA Student of the Year winners are all high achievers and ambassadors for the MBA, but another thing they have in common is the way they have utilised their MBA for the greater good. How are you planning to use your MBA? We are looking for highly-skilled and highly-motivated MBAs for the most sought-after accolade in the business education arena. The MBA Student of the Year Award comes with intense media exposure, the role of ambassador for the MBA and for the Association of MBAs and a £1,000 cash prize for the winner (£500 for the runners-up). Ask your school for details on the nominating process.
www.mbaworld.com/soty
3 3 3 3
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Meet admissions officers
Scholarships & funding information
en try !
Accredited MBA programmes only Free informative sessions
The Accredited
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Saturday 21 April Park Plaza Victoria Hotel, London, SW1V 1EQ Free sessions on MBA study from experts (including London Business School), advice on how to choose the right MBA programme for you, scholarships & funding, taking the GMAT, what employers look for in an MBA, PLUS prize giveaways. Register now: www.mbaworld.com/mbafair
Organised by:
INSPIRING GLOBAL EXCELLENCE
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Sponsored by:
INSPIRING GLOBAL EXCELLENCE
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The Association of MBAs
Conferences Awards Invites
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Juice Event Production
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Juice Event Production
Logo Design Branding Website Design
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Go on. Dive in. Make a splash. When you take a dip into the world of O2, you’ll be able to get more done, from more places, more easily than ever before. True our products don’t go underwater – yet. But, almost anywhere else you choose to work, chill-out or play, O2 will be there by your side. Take a closer look at the Xda II and see how it can support your life.
DIE CUT
It’s a truly global phone Want to make a call as you board a plane in New York and make another when you land London or Hong Kong? Can do. Tri-band capabilities cross countries and continents to keep you in touch. And, with a Bluetooth headset you’ll be doing it wireless and hands-free. If text’s your thing, you’ll find your SMS is now ‘LMS’, unlimited by the 160 character constraint in English or 67 character constraint in Chinese of other devices. It’s a powerful PC in your pocket A fast 400mhz Intel processor and plenty of memory which you can always expand – combine with the latest Windows MobileTM 2003 software to put you firmly in control.
It’s oh so connected With infrared, Bluetooth, SDIO and, optional Wi-Fi support, your Xda II can talk to an ever-expanding world of peripherals without wires.
It’s wired for the web worldwide Improved GPRS gets you online wherever you are in the world. Whatever you want to do on the web is easy, no matter how rich the content.
Print from a printer across the room, access your corporate network quickly and securely, back up files to your PC, surf the Internet from your armchair, or use a global positioning solution in your car to guide you to your destination. New and innovative applications are being developed all the time.
Email, powered by Pocket Outlook software, is simple and reliable. Add pictures and video to illustrate a business case or amuse family and friends. Or chat online in real time with instant messaging.
How about giving a PowerPoint presentation from your Xda II? All you need is the optional back pack accessory to hook up to a projector.
Create and update Word and Excel files on the run. Organise your notes, appointments and thousands of contacts. Display pdf files or review that all-important PowerPoint presentation. No problem.
It’s multi-multimedia Photograph a new product launch, video a production facility or capture a special moment. It’s easy. Xda II has a built in camera to shoot video and still images. And, with all that connectivity about, you can instantly email them or send a multimedia message (MMS) to colleagues and friends.
It looks great Just because it’s packed with functionality, don’t think we’ve forgotten the form. After all, your Xda II will be going everywhere with you so it’s got to look good too.
With all this and more, shouldn’t Xda II be your ultimate global mobile companion? Contact. Communicate. Connect. Capture. Chill.
Alternatively, just chill out and listen to the latest MP3 audio through the high quality stereo headset. Don’t worry you can still take that phone call at the touch of a button.
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Telefonica O2
XDA II Xphone
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Red Squirrel Survival Trust
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The Red Squirrel Survival Trust (RSST)
www.rsst.org.uk
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Angelina Colarusso
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Angelina Colarusso
www.angelinacolarusso.com
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The State Corporation for Spanish Cultural Action Abroad (SEACEX)
Year of Spain in China
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GTZ -The Deutsche Gesellschaft für Internationale Zusammenarbeit GmbH
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Festival of Australian Theatre in China (FAT)
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OneWedding
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onewedding
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Shangri-La International Hotel Management Ltd.
Bento & Berries Delicatessen
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AS Watson - Taste supermarkets
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Universal Music Group
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Universal Music Group
Promotional DVDs for Universal Music Group
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The Disney Music Group (DMG)
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The Disney Music Group (DMG) or formerly Buena Vista Music Group)
Promote DMGs various show and brand in house
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citigroup
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citigroup
Graduate programme for citigroup graduates
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Starbucks
S
STARBUCKS COFFEE ASIA PACIFIC
tarbucks
Food for
Coffee
STARBUCKS COFFEE ASIA PACIFIC ©2002 STARBUCKS COFFEE COMPANY ALL RIGHTS RESERVED.
©2002 STARBUCKS COFFEE COMPANY ALL RIGHTS RESERVED.
COMMITMENT TO
COMMITMENT TO
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1. PLANNING DOCUMENTS :: :: :: ::
© 2003 STARBUCKS COFFEE COMPANY ALL RIGHTS RESERVED.
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STARBUCKS COFFEE ASIA PACIFIC © 2003 STARBUCKS COFFEE COMPANY. ALL RIGHTS RESERVED. CONFIDENTIAL - DO NOT REPRODUCE OR COPY.
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Starbucks Corporation
Commitment to Origins (CTO) Starbucks Food Toolkit
Brand localization Online Marketing Mixed Media
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Nick Ng
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Nick Ng
Art Exhibition
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97 Group
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ninetysevengroup
Design conceptualization Promtional Flyers
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Promotional
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Annie + Patrick
Wedding Invitation
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CLIENT
Imanova
CLIENT
PROJECT
WORK TYPE
Abbott
FreeStyle Libre marketing material
• Editorial Layouts • Social Media Content • Gifs • New Business Visualisations
• E-Marketing Designs • PowerPoint Presentations • Website Design • Infographics