Pharmacogenetics of Efavirenz: Adherence and Virologic Outcomes

  1. Jean B. Nachega, MD, MPH; and
  2. Gary Maartens, MBChB
  1. From Johns Hopkins University, Baltimore, MD 21205, and University of Cape Town, 7925 Cape Town, South Africa.

    IN RESPONSE:

    We thank Dr. Cennimo for bringing up this interesting point. The primary aim of our analysis was to assess the relationship between adherence and virologic outcomes on NNRTI regimens, and we caution that our finding of superior outcomes for efavirenz compared with nevirapine must be regarded as preliminary.

    The homozygous CYP2B6 position 516 TT genotype was found in 3.4% of European Americans and 20% of African Americans in the AIDS Clinical Trials Group study A5097s (1), close to 50% in participants in a study from Ghana (2), and 13.1% of participants in a recent South African study (3). The CYP2B6 TT genotype increases the efavirenz half-life, but as pointed out in the article Dr. Cennimo cites (4), this would be expected to result in a higher risk for drug-resistant mutations in poorly adherent patients, because the interruption of other antiretroviral drugs with shorter half-lives will result in prolonged effective monotherapy with efavirenz.

    The CYP2B6 TT genotype is also associated with an increased incidence of efavirenz-induced neuropsychiatric symptoms (1), which may reduce adherence. Therefore, one could argue that efavirenz should be associated with poorer outcomes in populations, such as that in our study, with a relatively higher proportion of patients with the CYP2B6 TT genotype. Finally, efavirenz has also been shown to be more effective than nevirapine in a collaborative study of 12 cohorts from Europe and North America (5) and in recent study of U.S. Veterans Affairs patients (6), populations in which the prevalence of the CYP2B6 TT mutation is low. This suggests that population pharmacogenetic differences are not the likely explanation for our preliminary finding that efavirenz is more effective than nevirapine.

     
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    Jean B. Nachega, MD, MPH

    Johns Hopkins University

    Baltimore, MD 21205

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    Gary Maartens, MBChB

    University of Cape Town

    7925 Cape Town, South Africa

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    Article and Author Information

    • Potential Financial Conflicts of Interest:Honoraria: J.B. Nachega (GlaxoSmithKline, Merck-Sharp-Dohme for continuing medical education lectures), G. Maartens (Merck-Sharp-Dohme). Grants received: G. Maartens (Merck-Sharp-Dohme). Other: J.B. Nachega (Aspen Pharmaceuticals for conferences and travel grants).

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    Summary for Patients

    • Article:Adherence to Nonnucleoside Reverse Transcriptase Inhibitor–Based HIV Therapy and Virologic Outcomes
      • Jean B. Nachega,
      • Michael Hislop,
      • David W. Dowdy,
      • Richard E. Chaisson,
      • Leon Regensberg,
      • and Gary Maartens
      Ann Intern Med April 17, 2007 146:564-573
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    1. Ann Intern Med December 4, 2007 vol. 147 no. 11 817-818
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