对有艾滋病进展高风险的无症状HIV感染受试者每日两次服用齐多夫定：一项随机、双盲、安慰剂对照研究。欧洲-澳大利亚协作组（研究017）

Zidovudine twice daily in asymptomatic subjects with HIV infection and a high risk of progression to AIDS: a randomized, double-blind placebo-controlled study. The European-Australian Collaborative Group (Study 017).

作者信息

Mulder J W, Cooper D A, Mathiesen L, Sandström E, Clumeck N, Gatell J M, French M, Donovan B, Gray F, Yeo J M

机构信息

Slotervaatziekenhuis, Department of Internal Medicine, Amsterdam, The Netherlands.

出版信息

AIDS. 1994 Mar;8(3):313-21. doi: 10.1097/00002030-199403000-00004.

DOI:10.1097/00002030-199403000-00004

PMID:7913326

Abstract

OBJECTIVE

To evaluate the efficacy of zidovudine given twice daily in subjects with asymptomatic HIV-1 infection and a high risk of progression to AIDS.

DESIGN

Randomized, double-blind placebo-controlled trial.

SETTING

Multicentre study in five European countries and Australia.

PATIENTS

Asymptomatic subjects (n = 329) with CD4 cell counts between 200 and 400 x 10(6)/l, or if > 400 x 10(6)/l, subjects with HIV p24 antigenaemia (> 10 pg/ml).

INTERVENTION

Patients were randomly assigned to receive zidovudine 500 mg or placebo twice daily for 104 weeks, following a 250 mg four times daily dose regimen for the first 4 weeks.

MAIN OUTCOME MEASURES

The primary end-point was the development of AIDS or severe AIDS-related complex (ARC). Before unblinding the study other end-points were defined: the development of Centers for Disease Control and Prevention (CDC) group IV disease (AIDS, severe ARC and other CDC stage IV disease) and the development of symptomatic HIV disease (AIDS, severe ARC, other CDC stage IV disease and minor HIV disease). Changes in CD4+ cell counts, p24 antigenaemia and toxicity were also reviewed.

RESULTS

Median treatment duration was 57 weeks for the placebo and 60 weeks for the zidovudine group, respectively. Progression to AIDS or severe ARC occurred in 17 placebo and 12 zidovudine recipients (log-rank P = 0.26). However, in the first of the 2 study years the rate of progression to AIDS or severe ARC was significantly higher in the placebo than in the zidovudine group. Zidovudine delayed progression to symptomatic HIV disease (P = 0.01); a trend in a delay in progression to CDC stage IV disease was observed (P = 0.08). Zidovudine recipients maintained CD4+ cell counts at or above baseline levels for longer than placebo recipients (P = 0.04). HIV p24-antigen levels decreased in the zidovudine group and returned to pretreatment levels by week 36. Substantial toxicity was not observed.

CONCLUSIONS

Zidovudine twice daily is effective in delaying progression to symptomatic HIV disease in high-risk, asymptomatic HIV-infected subjects. Modified definitions of clinical end-points may be useful for evaluating Phase III trials in comparable patient groups in the light of changes in the definition of AIDS and the increasing use of primary prophylaxis against opportunistic infections.

摘要

目的

评估每日两次服用齐多夫定对无症状HIV-1感染且有高进展至艾滋病风险的受试者的疗效。

设计

随机、双盲、安慰剂对照试验。

地点

在五个欧洲国家和澳大利亚进行的多中心研究。

患者

无症状受试者（n = 329），CD4细胞计数在200至400×10⁶/l之间，或者如果CD4细胞计数>400×10⁶/l，则为HIV p24抗原血症（>10 pg/ml）的受试者。

干预

患者在最初4周每日四次服用250 mg剂量方案后，被随机分配接受每日两次500 mg齐多夫定或安慰剂，持续104周。

主要结局指标

主要终点是艾滋病或严重艾滋病相关综合征（ARC）的发生。在揭盲研究之前定义了其他终点：疾病控制和预防中心（CDC）IV组疾病（艾滋病、严重ARC和其他CDC IV期疾病）的发生以及有症状HIV疾病（艾滋病、严重ARC、其他CDC IV期疾病和轻度HIV疾病）的发生。还评估了CD4⁺细胞计数、p24抗原血症和毒性的变化。

结果

安慰剂组的中位治疗持续时间为57周，齐多夫定组为60周。17名安慰剂组受试者和12名齐多夫定组受试者进展为艾滋病或严重ARC（对数秩检验P = 0.26）。然而，在研究的第1个年份，安慰剂组进展为艾滋病或严重ARC的发生率显著高于齐多夫定组。齐多夫定延迟了有症状HIV疾病的进展（P = 0.01）；观察到有进展至CDC IV期疾病延迟的趋势（P = 0.08）。齐多夫定组受试者维持CD4⁺细胞计数在基线水平或以上的时间比安慰剂组受试者更长（P = 0.04）。齐多夫定组HIV p24抗原水平下降，到第36周时恢复到治疗前水平。未观察到严重毒性。