Quality-of-Life Evaluation in a Clinical Trial of Zidovudine Therapy in Patients with Mildly Symptomatic HIV Infection

  1. Richard D. Gelber, PhD;
  2. William R. Lenderking, PhD;
  3. Deborah J. Cotton, MD, MPH;
  4. Bernard F. Cole, PhD;
  5. Margaret A. Fischl, MD;
  6. Aron Goldhirsch, MD; and
  7. Marcia A. Testa, PhD
  1. AIDS Clinical Trials Group

    Abstract

    Objective: To evaluate the effects of zidovudine therapy in patients with mildly symptomatic HIV infection using Q-TWiST (quality-adjusted: Time Without Symptoms and Toxicity).

    Design: Analysis of a previously reported multicenter, randomized, placebo-controlled clinical trial.

    Setting: Thirty-two AIDS Clinical Trial units.

    Patients: A total of 351 patients with mildly symptomatic HIV infection were assigned to placebo, and 360 patients were assigned to zidovudine, 1200 mg/d.

    Measurements: A modified Q-TWiST method for comparing treatments based on time spent without severe symptomatic adverse events and without disease progression. Zidovudine and placebo were compared in a threshold utility analysis considering reduction in quality of life associated with adverse events and disease progression. Adverse events defined by laboratory findings were distinguished from findings representing symptomatic events.

    Results: The incidence of severe symptomatic adverse events was 22.8% for the zidovudine group and 15.1% for the placebo group (P = 0.01), but, as previously reported, zidovudine improved progression-free survival relative to placebo (at 18 months, 91% compared with 81%; P = 0.001). In an 18-month period, patients receiving zidovudine went an average of 14.5 months without disease progression or a severe symptomatic adverse event compared with 14.7 months for placebo. The zidovudine group gained 0.9 months without disease progression but lost 1.1 months due to adverse events. Within the 18-month observation period, treatment provided more Q-TWiST than placebo if the quality of life after HIV disease progression was assumed to be 10% to 20% worse than the quality of life after a severe symptomatic adverse event.

    Conclusions: The Q-TWiST analysis projects that quality-of-life reductions due to severe symptomatic adverse events might be balanced by the quality-of-life benefits of delayed HIV disease progression for patients who receive zidovudine for mildly symptomatic HIV infection. At currently recommended doses (500 to 600 mg/d, half the dose used in this study) zidovudine therapy is likely to yield a more favorable result.

    Article and Author Information

    • For current author affiliations and addresses, see end of text.

    • Grant Support: In part by grant PBR-53 from the American Cancer Society and by contract NO-Al-95030 for the Statistical and Data Analysis Center of the AIDS Clinical Trials Group, Division of AIDS, National Institute of Allergies and Infectious Diseases, National Institutes of Health, Department of Health and Human Services.

    • Requests for Reprints: Richard D. Gelber, PhD, Division of Biostatistics and Epidemiology, Dana-Farber Cancer Institute, Mayer 432, 44 Binney Street, Boston, MA 02115.

    • Current Author Addresses: Drs. Gelber and Cole: Division of Biostatistics and Epidemiology, Dana-Farber Cancer Institute, Mayer 432, 44 Binney Street, Boston, MA 02115.

      Drs. Lenderking, Cotton, and Testa: Statistical and Data Analysis Center, Harvard School of Public Health, 677 Huntington Avenue, Boston, MA 02115.

      Dr. Goldhirsch: Department of Oncology, Ospedale Civico, Lugano, Switzerland.

      Dr. Fischl: Department of Medicine, University of Miami School of Medicine, Jackson Memorial Hospital, P.O. Box 016960, R-60A, Miami, FL 33101.

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    1. Ann Intern Med June 15, 1992 vol. 116 no. 12 Part 1 961-966
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