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2009 Revisions of WHO recommendations on use of Antiretroviral Therapy (ART)

2009 Revisions of WHO recommendations on use of Antiretroviral Therapy (ART). This a draft ! HIV/ATC October 2009. WHO ART treatment guidelines –the critical issues being reviewed. How to diagnose earlier? . Critical patient & public health important outcomes: Mortality

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2009 Revisions of WHO recommendations on use of Antiretroviral Therapy (ART)

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  1. 2009 Revisions of WHO recommendations on use of Antiretroviral Therapy (ART) This a draft ! HIV/ATC October 2009

  2. WHO ART treatment guidelines –the critical issues being reviewed How to diagnose earlier? • Critical patient & public health important outcomes: • Mortality • Disease progression (morbidity) • Severe or regimen limiting adverse events • Adherence & retention on ART • Durability of regimen effect • Reduction of HIV transmission • Cost • Other outcomes evaluated: • CD4 • HIV viral load • HIV drug resistance • HBV drug resistance & viral load How to monitor? When to Start? What to Use 1st Line? What to use- 2nd Line? Third line ?

  3. Major Populations being considered • HIV+ve Adults & adolescents • HIV+ve Pregnant Women • HIV+ve with TB Co-Infection • HIV+ve with Hepatitis B co-Infection

  4. Drafting Recommendations: Risk Benefit Analysis • Systematic reviews and GRADE profiles • Impact assessment reports • PLWH consultation reports • Costing and feasibility analysis DRAFT RECOMMENDATIONS PEER REVIEW FINAL RECOMMENDATIONS Panel at all times valued highly avoidance of death, HIV disease progression and severe adverse events

  5. Quality of evidence The extent to which one can be confident that an estimate of effect or association is correct.

  6. Strength of recommendation The degree of confidence that the desirable effects of adherence to a recommendation outweigh the undesirable effects. • Desirable effects • Health benefits • Improved quality of life • Cost efficiencies • Undesirable effects • Adverse outcomes • Decreased quality of life • Increasing health costs

  7. General principles • Put best option first then, what to do if best option not available • Be clear when strong evidence warrants strong recommendation • Be explicit if limited data available to support recommendations • Be somewhat aspirational – recognize what will likely be required & possible over next few years

  8. Proposed WHO 2009 Criteria for the ART Initiation in adults and adolescents(ART Guidelines Meeting, October/2009)

  9. Proposed WHO 2009 Preferred Regimens for ART Initiation in adults and adolescents(ART Guidelines Meeting, October/2009)

  10. Choosing among first line ART options in adults and adolescents(ART Guidelines Meeting, October/2009) AZT or TDF + (3TC/FTC) + NVP or EFV • No clear evidence to support TDF over and above AZT • Countries encouraged to minimize the number of options and select the preferred regimen likely to cover the majority of ARV naive population eligible for treatment. • Use of FDC formulations strongly recommended. • Adaptation guide will be critical to assist countries in developing own ART recommendations; the principle of “first do no harm” and equity & feasibility should be paramount in decision making. • Countries need to establish phase out plan for d4T as preferred 1st line NRTI and undertake risk assessment for continued use; low dose d4T has a role as backup option in case of AZT or TDF toxicity or other contraindications. • ABC removed as 1st line option.

  11. Recommendations on When to Start & What to Use in Pregnancy, TB/HIV and HBV/HIV • Pregnancy: • Benefits of NVP for women with CD4 cell count between 250 to 350/mm3 likely to outweigh risk of not treating. • EFV regimens preferred but low risk of NTD (<1%) means should avoid starting in first trimester. • AZT regimens preferred in pregnancy but TDF appears safe acceptable alternative. • TB/HIV: • EFV based regimens preferred initial options. • All active TB start ART as soon as tolerated. • Rifabutin in TB regimen if using concomitant PI regimen. • HBV/HIV: • TDF/3TC or TDF/FTC as preferred NRTI backbone. • If active HBV disease start ART irrespective of CD4 cell count.

  12. Choice of ART regimen for HIV+ women with prior exposure to MTCT regimens

  13. Recommendations on Lab Monitoring • Recognise and describe the following phases of HIV management : • Hb recommended prior to AZT use. • TDF can be used in absence of renal screening or monitoring (benefits outweigh the risks). • Symptom directed laboratory monitoring for toxicity is recommended. • Simplified algorithms for ART failure being developed and evaluated. • Viral load threshold of 5000 copies /ml used for detect or confirm treatment failure.

  14. Other Recommendations • Countries will need to prioritize increased CD4 threshold, transition to safer 1st line drugs and targeted use of laboratory monitoring in the context of equity, sustaining scale up and quality of care.

  15. Proposed WHO 2009 2nd Line ART Regimens in adults and adolescents(ART Guidelines Meeting, October/2009) • Boosted PI based second line therapy is strongly recommended. • Which boosted PI to use should be decided based on cost and availability of products esp. heat stable FDCs, ATVr and LPVr are preferred options. • No clear benefits of using ATV/r over LPV/r . • NRTI options determined by first line –in general non thymidine based regimens lead to potentially more favourable NRTI options for second line.

  16. Third-line ART • Mortality for patients on failing second line ART is high . • Countries should develop a policy vis a vis third line options. • Countries should consider providing a 3rd line regimen for patients failing 2nd line ART. • Countries should consider using boosted darunavir plus raltegravir and/or etravirine as third line drugs if available. • If 3rd line drugs are not available, the failing 2nd line regimen should be continued if tolerated, or previously used drugs recycled based on tolerance.

  17. Next Steps • Meeting Report • Develop adaptation/transition guide (Prof James Hakim will host working meeting to draft, Mid November, Harare) • Develop draft of revised 2009 Guideline • Review by guideline panel group & peer review group • d4T phase out and risk assessment tool (to be developed by WHO) • Issues to be reviewed/verified: • WHO clinical stage 2 – data on CD4 distribution and progression by condition (some stage 2 seems to be more “severe” than others) • Use of high dose folate to reduce risk of neural tube defects if EFV used in women of reproductive age. • How to prioritize introduction of revisions, notably increasing the CD4 threshold vs. transitioning away from d4T? • Low dose d4T dosing • Hep B - definition and assessment of active chronic hepatitis in RLS • Hep C - check if when or what ART to use changes if on Rx?

  18. Final Comments • Some slight changes in relation to 2006 Guidelines. • Trends: • Encourage earlier diagnosis • Treat earlier • Promote less toxic/ more friendly regimens • Monitor more strategically • Will cost more • The major operational question is not if these recommendations should be followed or not, but how to do it safely and with equity… • Burning unresolved issues - lack of WHO guideline for Hepatitis B and C management.

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