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Drug Treatment Regimens: How and why WHO makes its global recommendations

Drug Treatment Regimens: How and why WHO makes its global recommendations. Prof Charles Gilks Director, Co-ordinator Antiretroviral Treatment and Care Department of HIV/AIDS WHO Geneva. WHO Drug Treatment Regimens.

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Drug Treatment Regimens: How and why WHO makes its global recommendations

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  1. Drug Treatment Regimens:How and why WHO makes its global recommendations Prof Charles Gilks Director, Co-ordinator Antiretroviral Treatment and Care Department of HIV/AIDS WHO Geneva.

  2. WHO Drug Treatment Regimens • Why WHO needed to make recommendations and to set global norms and standards • How WHO set about doing this • Consider how successful or not WHO's work has been in ART scale-up so far • Revised (2008) WHO processes for making recommendations and issuing guidance

  3. “Three by Five” 2002 / 2003: GFATM and PEPFAR established and resourced The target: three million people on treatment by the end of 2005 The goal : universal access to anti- retroviral therapy (ART) as a human right to health to all in need The treatment gap was declared a global health emergency Sept 22nd, 2003 at UN General Assembly

  4. Filling the treatment gap • WHO entered "emergency mode" • Defined the extent of the problem • end 2002, estimated 300,000 on ART • 91% of treatment gap in 34 countries • Recognised the extent of the challenge • New intervention with limited experience • Countries most in need had weakest health systems • Prevailing view: ART was complex and specialised

  5. Delivering on 3 x 5 • WHO’s strategy: to catalyse rapid uptake of ART in communities where it is needed now but not widely accessible by adopting a two-pronged approach: • Supporting countries to recognise and respond to their HIV/AIDS treatment gap and leveraging the necessary resources to enable ART to be scaled up rapidly in line with 3x5 target • Simplifying and standardizing ART as • far as possible without compromising effectiveness so it can be universally scaled up and delivered in resource constrained settings

  6. Vision: Universal access to ART Elements: One global standard of care for ART One first-line then one second-line regimen (then stop) Sequential use of 3 drug classes Simple recommendations for when to start switch & toxicity substitutions Tiered laboratory support for clinical decision-making Standard population-based HIVDR monitoring and surveillance Pharmacovigilance/toxicity monitoring Chronic disease management Integrated and decentralised care Process: Evidence-based Simplification Standardisation Public Health ART Strategy

  7. Harmonised ART Policy Guidance

  8. Audience for guidelines • Primarily national planners and policy makers engaged in public sector ART and in target-setting • What ARVs to make available in public sector first and second-line regimens • How to use: the four Ss of clinical management: when to start, substitute, switch and stop • Care implementers - basic knowledge to use ARVs effectively according to national policy recommendations • Trainers, M&E experts – to design appropriate tools and materials to support national policy recommendations

  9. 1st and 2nd line ARVs for adults 1st Line 2nd line Start Substitute Switch Stop AZT, d4T, 3TC, NVP; EFV ddI PI/r ABC, TDF Frequently Recommended as 2nd line drugs, but also as alternative drugs in 1st line regimens Recommended 1st Line ARV Drugs Recommended as 2nd Line Drugs

  10. When to Start - adults

  11. Clinical Virologic Immunologic Failure / When to Switch Clinical criteria CD4 count Viral load "Early Switch" "Late Switch"

  12. When to Switch from 1st Line to 2nd Line ARV Regimens for Treatment Failure Clinical failure is defined as a occurrence of new or recurrent WHO clinical stage 3 or 4 event (excluding IRIS). CD4 failure is defined as a fall to (or below) the pre-treatment baseline or a 50% drop from the on-treatment peak level or persistent levels < 100 cells/mm3. Virological failure is provisionally defined as a plasma HIV-1 RNA level >10,000 copies/ml after a minimum of 6 months on therapy.

  13. Country HIVDR Committees HIVDR monitoring & surveys The WHO HIVResNet is a global group of experts, laboratories, and organizations constituted to support HIVDR prevention, surveillance, and monitoring as antiretroviral treatment (ART) is rolled out worldwide. Steering Committee WHO Secretariat • WHO HIVResNet • Laboratory Network • Surveillance and Monitoring Network WG Modeling of The emergence and transmission of resistance WG Operational Research Time-Limited Subject Matter Working Groups WG Mutation lists for Surveillance and monitoring WG WG Global Laboratory Network: Criteria, Protocols, Training, QA HIVDR database development and support WG Public Health Assessment Tool For evaluation of country HIVDR data

  14. 2005 G8 Summit at Gleneagles, Final Communiqué: “…working with WHO, UNAIDS and other international bodies to develop and implement a package of HIV prevention, treatment and care, with the aim of as close as possible to universal access to treatment for all those who need it by 2010.” Universal Access

  15. Progress has been made with children • More children are receiving ART • Increased from 75,000 in 2005 to almost 200,000 in 2007 Towards Universal Access: Scaling up priority HIV/AIDS interventions in the health sector, WHO/UNAIDS/UNICEF 2008

  16. Revised simplified dosing

  17. WHO FDC ARV tablet regimen superimposed 1 ADULT FDC AM & PM 1 ADULT FDCAM & 0.5 PM 0.5 ADULT FDC AM + PM 2 BABY FDC AM & PM 2 BABY FDC AM & 1 PM 1 BABY FDC AM & 1 PM Most dose adjustments done in 1st year Same dosing irrespective of FDC, or same dosing for all three single ARV agents Adapted from T. NUNN

  18. Revised (2008) WHO process • New WHO Guideline review committee • Revised WHO guidelines for guidelines • Minimum standards for: • Reporting • Processes • Use of evidence • Different types of guidance documents recognised to fit different purposes: E.g. Emergency, Standard, Full , 'Books ' joint guidelines?

  19. Quality of evidence – GRADE approach

  20. Strength of a recommendation

  21. Conclusions • Developing WHO drug treatment regimens is challenging – but can have great impact • Balance between • being permissive; driving ART agenda forward • maintaining relevance to all countries • Processes updated in WHO (GRADE) • Even more rigorous and transparant • Costs and feasibility

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