Two Controlled Trials of Rifabutin Prophylaxis against Mycobacterium avium Complex Infection in AIDS

doi:10.1056/NEJM199309163291202

Volume 329:828-833		September 16, 1993		Number 12

Two Controlled Trials of Rifabutin Prophylaxis against Mycobacterium avium Complex Infection in AIDS

Stephen D. Nightingale, D. William Cameron, Fred M. Gordin, Paul M. Sullam, David L. Cohn, Richard E. Chaisson, Lawrence J. Eron, Paula D. Sparti, Bernard Bihari, David L. Kaufman, John J. Stern, Daniel D. Pearce, Winkler G. Weinberg, Anthony LaMarca, and Frederick P. Siegal

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ABSTRACT

Background Disseminated Mycobacterium avium complex infectioneventually develops in most patients with the acquired immunodeficiencysyndrome (AIDS). This infection results in substantial morbidityand reduces survival by about six months.

Methods We conducted two randomized, double-blind, multicentertrials of daily prophylactic treatment with either rifabutin(300 mg) or placebo. All the patients had AIDS and CD4 cellcounts $<=$ 200 per cubic millimeter. The primary end point wasM. avium complex bacteremia as assessed monthly by blood culture.The secondary end points were signs and symptoms associatedwith disseminated M. avium complex infection, adverse events,hospitalization, and survival.

Results In the first trial, M. avium complex bacteremia developedin 51 of 298 patients (17 percent) assigned to placebo and 24of 292 patients (8 percent) assigned to rifabutin (P<0.001).In the second trial, bacteremia developed in 51 of 282 patientsin the placebo group (18 percent) and 24 of 274 patients inthe rifabutin group (9 percent) (P = 0.002). Rifabutin significantlydelayed fatigue, fever, decline in the Karnofsky performancescore (by $>=$ 20 percent), decline in the hemoglobin level (bymore than 10 percent), elevation in alkaline phosphatase, andhospitalization. The incidence of adverse events was similarwith rifabutin and placebo. Overall survival did not differsignificantly between the two groups, although there were fewerdeaths with rifabutin (33) than with placebo (47) during thedouble-blind phase (P = 0.086). The distribution of minimalinhibitory concentrations of rifabutin among the isolates ofM. avium complex did not differ significantly between the treatmentgroups.

Conclusions Rifabutin, given prophylactically, reduces the frequencyof disseminated M. avium complex infection in patients withAIDS and CD4 counts $<=$ 200 per cubic millimeter.

Source Information

From the University of Texas Southwestern Medical Center, Dallas (S.D.N.); Ottawa General Hospital, Ottawa, Ont. (D.W.C.); the Veterans Affairs Medical Center, Washington, D. ${beta}$ (F.M.G.); the Veterans Affairs Medical Center, San Francisco (P.M.S.); Public Health Administration and Disease Control, Denver (D.L.C.); Johns Hopkins School of Medicine, Baltimore (R.E.C.); Community Research Initiative of South Florida, Miami (P.D.S.); Community Research Initiative, New York (B.B.); the Pennsylvania Hospital, Philadelphia (J.J.S.); San Diego Community Research Group, San Diego, Calif. (D.D.P.); TheraFirst Medical Center, Fort Lauderdale, Fla. (A.L.); the Long Island Jewish Medical Center, New Hyde Park, N.Y. (F.P.S.); and private practice in Annandale, Va. (L.J.E.), New York (D.L.K.), and Atlanta (W.G.W.). Additional clinical investigators and study centers are listed in the Appendix.

Address reprint requests to Dr. Gordin at the Veterans Affairs Medical Center, 50 Irving St., NW, Washington, DC 20422.

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