Decreased monocyte activation with daily acyclovir use in HIV-1/HSV-2 coinfected women.

نویسندگان

  • Andrew D Redd
  • Kevin Newell
  • Eshan U Patel
  • Fred Nalugoda
  • Paschal Ssebbowa
  • Sarah Kalibbala
  • Melanie A Frank
  • Aaron A R Tobian
  • Ronald H Gray
  • Thomas C Quinn
  • David Serwadda
  • Steven J Reynolds
چکیده

OBJECTIVES Several clinical trials have demonstrated that daily treatment of HIV-infected individuals with the antiherpes drug acyclovir slightly decreases HIV-1 viral load and slows disease progression. This study examines if this slowing in clinical progression is a direct cause of the decrease in viral load or an indirect effect of lower immune activation due to lower levels of herpetic reactivation. METHODS Women who participated in a randomised clinical trial of daily acyclovir use (n=301) were monitored every 6 months for changes in immune activation. Soluble CD14 (sCD14), a marker for monocyte activation, and C-reactive protein (CRP), a marker for general immune activation, were measured by ELISA. RESULTS Initial levels of sCD14 and CRP were not predictive of HIV disease progression when controlling for initial CD4+ cell count and HIV viral load. sCD14 levels, but not CRP, decreased in the acyclovir treatment arm at a significantly faster rate than the placebo group, which was independent of changes in HIV viral load and CD4+ cell count in a multivariant mixed-effects model (p=0.039). However, the magnitude of this decrease was relatively small with a total estimated decrease of sCD14 of 15% of initial levels. CONCLUSIONS These data suggest that decreased monocyte activation may play a minor role in the ability of daily acyclovir use to slow HIV disease progression. CLINICAL TRIAL REGISTRATION NUMBER NCT00405821.

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عنوان ژورنال:
  • Sexually transmitted infections

دوره 91 7  شماره 

صفحات  -

تاریخ انتشار 2015