AI Article Synopsis

  • A study compared two different HIV treatment regimens: nelfinavir/nevirapine and ritonavir/saquinavir, both combined with two nucleoside reverse transcriptase inhibitors, involving 233 patients with no prior treatment.
  • After 48 weeks, 69% of patients on nelfinavir/nevirapine achieved low HIV RNA levels (≤20 copies/ml), compared to 56% on ritonavir/saquinavir, indicating that nelfinavir/nevirapine had better virological effects.
  • However, 44% of patients discontinued their assigned therapy, mainly due to side effects, highlighting the need for longer follow-up to assess potential long-term complications and drug resistance from these treatments.

Article Abstract

Background: A triple-class HAART regimen may be associated with a better virological effect than conventional regimens, but may also lead to toxicity and more profound resistance.

Methods: Randomized, controlled, open-label trial of 233 protease inhibitor- and non-nucleoside reverse transcriptase inhibitor-naive HIV-infected patients allocated to a regimen of nelfinavir and nevirapine (1250/200 mg twice daily; n = 118) or ritonavir and saquinavir (400/400 mg twice daily; n = 115), both in combination with two nucleoside reverse transcriptase inhibitors. The primary end-point was HIV RNA < or = 20 copies/ml after 48 weeks (missing value = failure). Patients remained under follow-up also in case of switch from the randomized therapy.

Results: At baseline, the median CD4 cell counts were 126 (range: 0-942) (nelfinavir/nevirapine) and 150 (0-642) (ritonavir/saquinavir) cells/mm3, and HIV RNA measurements 5.0 copies/ml (1.3-6.4) in both groups. A total of 102 (86%) and 101 (88%) were antiretroviral-naive. 44% discontinued randomized therapy; P = 0.13. Of these, 80 and 73% switched therapy due to adverse events; P = 0.99. At week 48, 69 and 56%, respectively, had a HIV RNA < or = 20 copies/ml; P = 0.037.

Conclusion: A regimen of nelfinavir/nevirapine had a favourable virological effect and tolerability over a 48-week period compared with ritonavir/saquinavir, when administered in combination with two nucleoside reverse transcriptase inhibitors. However, more extensive follow-up is required to determine the long-term consequences of triple class HAART regimens, including the development of broad drug resistance.

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