Bridging the gap between research, MCC approval and
public access to tenofovir gel
Quarraisha Abdool Karim
on behalf of the CAPRISA 008 & CAPRISA 009 teams
Parliamentary Portfolio Committee on Science & Technology
5 June 2013, Cape Town
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Tenofovir Gel since CAPRISA 004: Next Steps
• Confirmatory Trial – FACTS 001 For MCC & FDA approval and licensure
• Manufacture – ProPreven
• Normative Guidelines (WHO/UNAIDS draft)
• Implementation CAPRISA 008 – integration into family planning services CAPRISA 009 – treatment outcomes in women with HIV
• Preparing for Public Access Toolkit development for providers and users Community Advocacy Efforts
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Why does HIV continue to spread in South Africa?
AIDS 1992, 6:1535-1539
0
<9 10-14
Pre
vale
nce
(%
)
15-19 20-24 25-29 30-39 40-49
2
4
6
8
10
FemaleMale
>49
1990
Seroprevalence of HIV infection in rural South Africa
Quarraisha Abdool Karim, Salim S. Abdool Karim,Bipraj Singh*, Richard Short† and Sipho Ngxongo‡
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High rates of HIV among
key populations:
young women in
Africa
HIV in 15–24 year men and
women(2008–2011)
Young women have up to 8 times more
HIV than men
Source: Adapted from UNAIDS 2012
Zimbabwe
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Age Group (Years)
HIV Prevalence(N=1029)
≤16 8.4
17-18 18.6
19-20 25.4
21-22 32.8
23-24 44.8
HIV prevalence in young pregnant women
in rural Vulindlela, South Africa (2009-2012)
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Grassroots Advocacy EffortsSiyafuna
66
Key Goals of CAPRISA 008
1. Provide post-trial access to tenofovir gel for HIV uninfected CAPRISA 004 study participants and community volunteers (UNAIDS Guidance point 19)
2. Develop and assess an implementation model for tenofovir gel provision through family planning services- Quality Improvement Model- Comprehensive SRH services
3. Collect additional safety data on tenofovir gel
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CAPRISA 008: Implementing tenofovir gel in family planning clinics
• Tenofovir gel provided by Family Planning service nurses with
◦ DMPA, oral contraceptive and other method users – tenofovir gel provided every 3 months
◦ For Nur-isterate users – tenofovir gel provided every 2 months
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Components of the Toolkit
• Providers, Users, Marketing & Demand Creation
• Providers
“How to” Training Manual – SRH service provision to include tenofovir gel
Clinic procedures and systems to:
◦ Monitor safety, pregnancy and HIV
◦ Drug accountability & AE reporting
Counseling and support aids
Key information for M&E
Management of post-PrEP infection
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Current status of CAPRISA 008
• First participant enrolled on November 5, 2012
• 425 participants screened; 359 enrolled and in follow-up
• 43% of women enrolled are CAPRISA 004 high adherers
• 54/516 women from CAPRISA 004 became infected prior to initiation of CAPRISA 008 10.5% seroconversion rate Incidence rate of 3.8/100wy
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Goal of CAPRISA 009
• Follow-up of HIV infected participants from CAPRISA 004 (control & intervention arm) to compare: Disease progression Therapeutic outcomes using a tenofovir
containing treatment regimen Monitor drug resistance
• Target population: 119 seroconvertors at end of CAPRISA 004 54 post-004 seroconvertors Seroconvertors in CAPRISA 008
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Current status of CAPRISA 009
• All seroconvertors who agree are in follow-up and care in CAPRISA 002/ Acute Infection Study until ARV treatment eligible
• First patient initiated on ARV treatment in
CAPRISA 009 in June 2011; 34 initiated on ARV treatment 15 from the tenofovir gel arm
• 6 month treatment success rate – 88.9%
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Summary
• CAPRISA 008 provides an opportunity to generate evidence for implementation that will be required when a licensed product is available Inclusion of research naïve volunteers from community
completes ethical obligations and adds value to experience
• CAPRISA 009 will provide additional safety data post-infection following exposure to tenofovir and provide data on concerns about drug resistance and therapeutic options for post-PrEP seroconvertors
• Toolkit based on experiences and outcomes from 008 and 009 will enable rapid introduction and scale-up of a licensed product
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Conclusions
• Tenofovir gel potentially adds a new approach to empower women to take control of their own risk of HIV infection
• CAPRISA 004 is the first step – it is likely that with time other products and formulations will surpass tenofovir gel
• Post-trial access of tenofovir gel through CAPRISA 008 provides an opportunity to generate evidence for implementation that will fast track the timelag between potential licensure and public access
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Acknowledgements• Financial support:
USAID through CONRAD The South African Government’s Department of Science & Technology (DST) through
the Technology Innovations Agency (TIA) M-A-C AIDS fund through the Tides Foundation
• Trial Oversight Committee: CAPRISA: Q Abdool Karim, SS Abdool Karim, LE Mansoor USAID (US): D Stanton, L Claypool USAID (Pretoria): R Fertziger CONRAD: H Gabelnick, G Doncel DST/TIA: S Gumbi, G Loots M-A-C AIDS/Tides: N Mahon, A Flynn Gilead Sciences: J Rooney
• Tenofovir & placebo gel: Provided by CONRAD & Gilead Sciences
• FHI Statistical: M Chen
• CONRAD regulatory support: J Schwartz, J Schafer
• Research infrastructure & training: US NIH’s CIPRA Program & the Columbia University - Southern African Fogarty Training Program
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