PLoS ONE (Jan 2013)

Role of HIV infection duration and CD4 cell level at initiation of combination anti-retroviral therapy on risk of failure.

  • Sara Lodi,
  • Andrew Phillips,
  • Sarah Fidler,
  • David Hawkins,
  • Richard Gilson,
  • Ken McLean,
  • Martin Fisher,
  • Frank Post,
  • Anne M Johnson,
  • Louise Walker-Nthenda,
  • David Dunn,
  • Kholoud Porter,
  • UK Register of HIV

DOI
https://doi.org/10.1371/journal.pone.0075608
Journal volume & issue
Vol. 8, no. 9
p. e75608

Abstract

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BackgroundThe development of HIV drug resistance and subsequent virological failure are often cited as potential disadvantages of early cART initiation. However, their long-term probability is not known, and neither is the role of duration of infection at the time of initiation.MethodsPatients enrolled in the UK Register of HIV seroconverters were followed-up from cART initiation to last HIV-RNA measurement. Through survival analysis we examined predictors of virologic failure (2HIV-RNA ≥400 c/l while on cART) including CD4 count and HIV duration at initiation. We also estimated the cumulative probabilities of failure and drug resistance (from the available HIV nucleotide sequences) for early initiators (cART within 12 months of seroconversion).ResultsOf 1075 starting cART at a median (IQR) CD4 count 272 (190,370) cells/mm(3) and HIV duration 3 (1,6) years, virological failure occurred in 163 (15%). Higher CD4 count at initiation, but not HIV infection duration at cART initiation, was independently associated with lower risk of failure (p=0.033 and 0.592 respectively). Among 230 patients initiating cART early, 97 (42%) discontinued it after a median of 7 months; cumulative probabilities of resistance and failure by 8 years were 7% (95% CI 4,11) and 19% (13,25), respectively.ConclusionAlthough the rate of discontinuation of early cART in our cohort was high, the long-term rate of virological failure was low. Our data do not support early cART initiation being associated with increased risk of failure and drug resistance.