耐药性突变对挽救治疗病毒学应答的影响。瑞士HIV队列研究。

Impact of drug resistance mutations on virologic response to salvage therapy. Swiss HIV Cohort Study.

作者信息

Lorenzi P, Opravil M, Hirschel B, Chave J P, Furrer H J, Sax H, Perneger T V, Perrin L, Kaiser L, Yerly S

机构信息

AIDS Centre, Geneva University Hospital, Switzerland.

出版信息

AIDS. 1999 Feb 4;13(2):F17-21. doi: 10.1097/00002030-199902040-00001.

DOI:10.1097/00002030-199902040-00001

PMID:10202819

Abstract

OBJECTIVE

To assess the prognostic significance of drug-associated mutations in the protease and reverse transcriptase (RT) genes on virological response to salvage therapy.

PATIENTS

All patients from four centres of the Swiss HIV Cohort Study who were switched, between February and October 1997, to nelfinavir plus other antiretroviral drugs following failure of highly active antiretroviral therapy (HIV-1 RNA >1000 copies/ml after > 3 months).

METHODS

Direct sequencing of RT and protease genes derived from plasma RNA was performed in 62 patients before salvage therapy. Baseline predictors (drug-resistance mutations, drug exposure, clinical and biological parameters) of virological response after 4-12 weeks of therapy were assessed by linear regression analyses.

RESULTS

Patients had been treated with RT inhibitors and protease inhibitors for a median duration of 35.6 and 12.2 months, respectively. Baseline median CD4 cell count was 113 x 10(6)/l and HIV-1 RNA 5.16 log10 copies/ml. The median decrease of HIV-1 RNA was 0.38 log10; 32% of the patients showed > 1 log10 decrease. At baseline, 90% of the patients had RT inhibitor-resistance mutations with a median number per patient of four (range, 0-7). Primary and secondary protease inhibitor-resistance mutations were detected in 69% and 89% of the patients, respectively. The median number of total protease inhibitor-resistance mutations per patient was four (range, 0-9). In univariate analysis, virological response to salvage therapy was associated with number of RT inhibitors, primary and secondary protease inhibitor-resistance mutations, history of protease inhibitor use (duration and number), but not with clinical stage, HIV-1 RNA level or CD4 cell count. After adjustment for all variables, the number of RT inhibitor plus protease inhibitor-resistance mutations was the only independent predictor.

CONCLUSIONS

In patients with advanced HIV infection, the virological response to salvage therapy containing nelfinavir is best predicted by the number of baseline RT inhibitor plus protease inhibitor-resistance mutations.

摘要

目的

评估蛋白酶和逆转录酶（RT）基因中与药物相关的突变对挽救治疗病毒学应答的预后意义。

患者

瑞士HIV队列研究四个中心的所有患者，这些患者在1997年2月至10月期间，在高效抗逆转录病毒治疗失败后（>3个月后HIV-1 RNA>1000拷贝/ml）改用奈非那韦加其他抗逆转录病毒药物。

方法

对62例患者在挽救治疗前进行血浆RNA来源的RT和蛋白酶基因直接测序。通过线性回归分析评估治疗4至12周后病毒学应答的基线预测指标（耐药突变、药物暴露、临床和生物学参数）。

结果

患者接受RT抑制剂和蛋白酶抑制剂治疗的中位持续时间分别为35.6个月和12.2个月。基线CD4细胞计数中位数为113×10⁶/l，HIV-1 RNA为5.16 log₁₀拷贝/ml。HIV-1 RNA的中位数下降为0.38 log₁₀；32%的患者下降>1 log₁₀。基线时，90%的患者有RT抑制剂耐药突变，每位患者的中位数为4个（范围0至7个）。分别在69%和89%的患者中检测到原发性和继发性蛋白酶抑制剂耐药突变。每位患者总蛋白酶抑制剂耐药突变的中位数为4个（范围0至9个）。在单变量分析中，挽救治疗的病毒学应答与RT抑制剂数量、原发性和继发性蛋白酶抑制剂耐药突变、蛋白酶抑制剂使用史（持续时间和数量）有关，但与临床分期、HIV-1 RNA水平或CD4细胞计数无关。在对所有变量进行调整后，RT抑制剂加蛋白酶抑制剂耐药突变的数量是唯一的独立预测指标。