A Proof-of-concept Study of Short-cycle Intermittent Antiretroviral Therapy with a Once-daily Regimen of Didanosine, Lamivudine, and Efavirenz for the Treatment of Chronic HIV Infection

Overview

Journal J Infect Dis

Publisher Oxford University Press

Specialty Infectious Diseases

Date 2004 May 15

PMID 15143462

Citations 18

Authors

Mark Dybul

Elizabeth Nies-Kraske

Robin Dewar

Frank Maldarelli

Claire W Hallahan

Marybeth Daucher

Stephen C Piscitelli

Linda Ehler

Ann Weigand

Sarah Palmer

Julia A Metcalf

Richard T Davey

Diane M Rock Kress

April Powers

Ingrid Beck

Lisa Frenkel

Michael Baseler

John Coffin

Anthony S Fauci

Affiliations

Soon will be listed here.

Abstract

Background: We previously demonstrated that short-cycle structured intermittent therapy (SIT; 7 days without therapy followed by 7 days with antiretroviral therapy [ART]) with a ritonavir-boosted, indinavir-based, twice-daily regimen maintained suppression of plasma HIV viremia while reducing serum levels of lipids. Adherence to such a regimen may be problematic for certain patients.

Methods: Eight patients with a history of receiving combination ART that maintained suppression of plasma HIV RNA to <50 copies/mL received a once-daily SIT regimen of didanosine, lamivudine, and efavirenz.

Results: For 7 patients, suppression of plasma HIV RNA to <50 copies/mL was maintained for 60-84 weeks. Four patients with adequate samples had no evidence for an increase in plasma viremia for up to 72 weeks, by use of an assay with a limit of detection of <1 copy/mL. The lack of rebound viremia may be the result of the persistence of efavirenz in plasma on day 7 of the no-therapy period, as was detected in 7 of 7 patients. There was no significant change in CD4(+) T cell counts or serum hepatic transaminase or lipid levels.

Conclusion: A once-daily short-cycle SIT regimen maintained suppression of plasma HIV RNA while preserving CD4(+) T cell counts. Such a regimen may have importance in resource-limited settings where the monetary cost of continuous ART is prohibitive.

Citing Articles

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Treatment simplification in HIV-infected adults as a strategy to prevent toxicity, improve adherence, quality of life and decrease healthcare costs.

Nachega J, Mugavero M, Zeier M, Vitoria M, Gallant J Patient Prefer Adherence. 2011; 5:357-67.

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Rapid and persistent selection of the K103N mutation as a majority quasispecies in a HIV1-patient exposed to efavirenz for three weeks: a case report and review of the literature.

Polilli E, Parruti G, Cosentino L, Sozio F, Saracino A, Consorte A J Med Case Rep. 2010; 3:9132.

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Changes in lipids and lipoprotein particle concentrations after interruption of antiretroviral therapy.

Lampe F, Duprez D, Kuller L, Tracy R, Otvos J, Stroes E J Acquir Immune Defic Syndr. 2010; 54(3):275-84.

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