初治人群采用现代治疗方案时 HIV-1 耐药的发生率。

Incidence of HIV-1 drug resistance among antiretroviral treatment-naive individuals starting modern therapy combinations.

机构信息

Division of Infectious Diseases and Hospital Epidemiology, University Hospital Zurich, University of Zurich, Switzerland.

出版信息

Clin Infect Dis. 2012 Jan 1;54(1):131-40. doi: 10.1093/cid/cir728. Epub 2011 Nov 4.

DOI:10.1093/cid/cir728

PMID:22057700

Abstract

BACKGROUND

Estimates of drug resistance incidence to modern first-line combination antiretroviral therapies against human immunodeficiency virus (HIV) type 1 are complicated by limited availability of genotypic drug resistance tests (GRTs) and uncertain timing of resistance emergence.

METHODS

Five first-line combinations were studied (all paired with lamivudine or emtricitabine): efavirenz (EFV) plus zidovudine (AZT) (n = 524); EFV plus tenofovir (TDF) (n = 615); lopinavir (LPV) plus AZT (n = 573); LPV plus TDF (n = 301); and ritonavir-boosted atazanavir (ATZ/r) plus TDF (n = 250). Virological treatment outcomes were classified into 3 risk strata for emergence of resistance, based on whether undetectable HIV RNA levels were maintained during therapy and, if not, whether viral loads were >500 copies/mL during treatment. Probabilities for presence of resistance mutations were estimated from GRTs (n = 2876) according to risk stratum and therapy received at time of testing. On the basis of these data, events of resistance emergence were imputed for each individual and were assessed using survival analysis. Imputation was repeated 100 times, and results were summarized by median values (2.5th-97.5th percentile range).

RESULTS

Six years after treatment initiation, EFV plus AZT showed the highest cumulative resistance incidence (16%) of all regimens (<11%). Confounder-adjusted Cox regression confirmed that first-line EFV plus AZT (reference) was associated with a higher median hazard for resistance emergence, compared with other treatments: EFV plus TDF (hazard ratio [HR], 0.57; range, 0.42-0.76), LPV plus AZT (HR, 0.63; range, 0.45-0.89), LPV plus TDF (HR, 0.55; range, 0.33-0.83), ATZ/r plus TDF (HR, 0.43; range, 0.17-0.83). Two-thirds of resistance events were associated with detectable HIV RNA level ≤500 copies/mL during treatment, and only one-third with virological failure (HIV RNA level, >500 copies/mL).

CONCLUSIONS

The inclusion of TDF instead of AZT and ATZ/r was correlated with lower rates of resistance emergence, most likely because of improved tolerability and pharmacokinetics resulting from a once-daily dosage.

摘要

背景

由于缺乏基因耐药性检测（GRT）以及对耐药性出现时间的不确定，估计抗人类免疫缺陷病毒（HIV）1 型的现代一线联合抗逆转录病毒疗法的耐药发生率较为复杂。

方法

研究了五种一线组合（均与拉米夫定或恩曲他滨联合使用）：依非韦伦（EFV）加齐多夫定（AZT）（n = 524）；EFV 加替诺福韦（TDF）（n = 615）；洛匹那韦（LPV）加 AZT（n = 573）；LPV 加 TDF（n = 301）；利托那韦增效阿扎那韦（ATZ/r）加 TDF（n = 250）。根据治疗期间是否维持 HIV RNA 水平不可检测，以及治疗期间病毒载量是否＞500 拷贝/ml，将病毒学治疗结果分为耐药出现的 3 个风险分层。根据风险分层和检测时接受的治疗，从 GRT（n = 2876）中估计耐药突变的存在概率。根据这些数据，对每个个体进行耐药出现事件的推断，并使用生存分析进行评估。重复推断 100 次，中位数（2.5 至 97.5 百分位范围）总结结果。

结果

治疗开始后 6 年，EFV 加 AZT 显示所有方案中累积耐药发生率最高（16%）（＜11%）。经过混杂因素调整的 Cox 回归证实，与其他治疗相比，一线 EFV 加 AZT（参照）与耐药出现的中位风险更高：EFV 加 TDF（危险比[HR]，0.57；范围，0.42-0.76），LPV 加 AZT（HR，0.63；范围，0.45-0.89），LPV 加 TDF（HR，0.55；范围，0.33-0.83），ATZ/r 加 TDF（HR，0.43；范围，0.17-0.83）。三分之二的耐药事件与治疗期间可检测到的 HIV RNA 水平≤500 拷贝/ml 相关，只有三分之一与病毒学失败（HIV RNA 水平＞500 拷贝/ml）相关。