Publication | Open Access
Role of Structured Treatment Interruption before a 5‐Drug Salvage Antiretroviral Regimen: The Retrogene Study
74
Citations
26
References
2003
Year
Virus SuppressionSalvage RegimenTreatment And PreventionRetrogene StudyHuman RetrovirusImmunologyStructured Treatment InterruptionResistance Mutation (Virology)VirologyAntiviral TherapyPharmacotherapyChronic Viral InfectionAntiviral DrugHivImmunotherapyMedicineSalvage Antiretroviral Regimen
We evaluated the efficacy of a 5-drug salvage regimen, preceded by a 12-week, structured treatment interruption (STI), in 46 multidrug-treated, human immunodeficiency virus type 1-infected patients with detectable viremia. Patients were randomly assigned to receive a 5-drug salvage regimen immediately (noninterruption [NI] group; n=24 patients) or after 12 weeks of STI (interruption [I] group; n=22 patients). At week 48, 45% of patients in the I group and 46% of patients in the NI group had virus loads <50 HIV-1 RNA copies/mL (P=.619). No differences in CD4 cell counts were seen between groups at week 48 (P=.734). A complete reversion to wild-type genotype was detected in 35% of patients in the I group, but this phenomenon did not affect the virological response. The only overall baseline factor associated with ensuing virus suppression was a lower number of nucleoside reverse-transcriptase inhibitor-resistant mutations (relative risk, 0.66; 95% confidence interval, 0.47-0.93; P=.021). A prior STI seems to confer no additional benefit to subsequent virological or immunological outcomes of a salvage regimen.
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