CLINICAL CORRELATES OF INVITRO HIV-1 RESISTANCE TO ZIDOVUDINE - RESULTS OF THE MULTICENTER CANADIAN AZT TRIAL

被引：90

作者：

MONTANER, JSG

SINGER, J

SCHECHTER, MT

RABOUD, JM

TSOUKAS, C

OSHAUGHNESSY, M

RUEDY, J

NAGAI, K

SALOMON, H

SPIRA, B

WAINBERG, MA

机构：

[1] MONTREAL GEN HOSP, MONTREAL H3G 1A4, QUEBEC, CANADA

[2] MCGILL UNIV, CTR AIDS, MONTREAL H3A 2T5, QUEBEC, CANADA

[3] UNIV BRITISH COLUMBIA, FAC MED, DEPT HLTH CARE & EPIDEMIOL, VANCOUVER V6T 1W5, BC, CANADA

[4] CENTR EXCELLENCE HIV & RELATED DIS, VANCOUVER, BC, CANADA

[5] CANADIAN HIV TRIALS NETWORK, VANCOUVER, BC, CANADA

[6] SIR MORTIMER B DAVIS JEWISH HOSP, LADY DAVIS INST, MONTREAL H3T 1E2, QUEBEC, CANADA

来源：

AIDS | 1993年 / 7卷 / 02期

关键词：

DRUG RESISTANCE; ZIDOVUDINE; HIV; DISEASE PROGRESSION;

D O I：

10.1097/00002030-199302000-00006

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Objective: To describe the rate of development of in vitro HIV resistance to zidovudine (ZDV) and its prognostic implications within the Multicentre Canadian AZT Trial (MCAT). Methods: HIV-infected subjects in Centers for Disease Control (CDC) stages IIB, III and IVC-2 with CD4 cell counts > 270 x 10(6)/l were treated with ZDV as part of a dose-range study. Participating volunteers underwent prospective clinical and laboratory evaluations at regular intervals. Viral cultures and sensitivity testing were performed every 12 weeks in a predefined subset of 50 volunteers. An isolate was designated ZDV-resistant if it had a median inhibitory concentration (IC50) for ZDV at least 50-fold higher than that of virus isolated from the same subject before initiation of antiviral chemotherapy. The relationship between resistance and subsequent disease progression was studied using the Mantel and Byar method, for which, at each instance of disease progression, 2 x 2 tables classifying progression versus resistance status were constructed. The observed number of progressions was compared with that expected under the null hypothesis using Mantel-Haenszel methods adjusted for baseline CD4:CD8 ratio. Results: The Kaplan-Meier estimate for the cumulative development of in vitro resistance was 64% [95% confidence interval (CI), 41-78] at 180 weeks. Baseline CD4:CD8 ratio was negatively associated (P = 0.10) with the subsequent development of resistance (proportional hazard, 0.44; 95% CI, 0.17-1.10). After adjusting for baseline CD4:CD8 ratio, the numbers of observed and expected progressions following the development of resistance were 15 and 7.6, respectively (P = 0.008). A similar relative risk of progression between resistant and non-resistant states was found in the two CD4:CD8 strata; observed and expected progressions were 4 and 2.3 and 11 and 5.2 in the high and low CD4:CD8 strata, respectively. Conclusions: In vitro resistance to ZDV developed in 64% of subjects after 180 weeks of ZDV therapy. Lower CD4:CD8 ratio at baseline was associated with faster development of resistance. In addition, the development of resistance was found to be a marker of subsequent disease progression. This association persisted after adjustment for baseline CD4:CD8 ratio. Whether in vitro resistance to ZDV is merely a surrogate marker or a determinant of disease progression remains to be established.

引用

页码：189 / 196

页数：8

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