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在一个大型的意大利耐药数据库(ARCA)中,对依曲韦林(TMC125)的突变和基因型耐药决定因素的流行情况。

Prevalence of mutations and determinants of genotypic resistance to etravirine (TMC125) in a large Italian resistance database (ARCA).

机构信息

Sezione Malattie Infettive e Immunopatologia, Dipartimento di Scienze Cliniche 'Luigi Sacco', Universita' degli Studi, Milan, Italy.

出版信息

HIV Med. 2010 Sep;11(8):530-4. doi: 10.1111/j.1468-1293.2009.00819.x. Epub 2010 Mar 8.

Abstract

OBJECTIVES

To evaluate whether etravirine (TMC125) might be effective in patients failing therapy with current nonnucleoside reverse transcriptase inhibitors (NNRTIs), we analysed the prevalence of TMC125 mutations and the possible determinants of genotypic resistance to this drug among sequences reported to a large database in Italy [Antiretroviral Resistance Cohort Analysis (ARCA)].

METHODS

We analysed the prevalence of TMC125 resistance-associated mutations (RAMs) and the TMC125 weighted genotypic score (WGS) together with the determinants of genotypic resistance. A total of 5011 sequences from 2955 patients failing NNRTI therapy were evaluated.

RESULTS

Among the sequences in ARCA, 68% had at least one and 9.8% at least three TMC125 RAMs, whereas 31% had a WGS>2. Frequent RAMs were Y181C, G190A, K101E and A98G, whereas V179F, Y181V and G190S appeared in <5% of sequences. Multivariate analysis revealed a higher risk of developing at least three TMC125 RAMs associated with both nevirapine and efavirenz exposure, whereas CD4 counts > or = 200 cells/microL retained their protective effect. An increased risk of WGS>2 was linked to higher HIV RNA values (maximum risk at >5 log(10) copies/mL) and nevirapine exposure; CD4 counts > or = 200 cells/microL were protective.

CONCLUSIONS

The prevalence of TMC125 resistance mutations in the ARCA cohort was 68%. The DUET studies showed that at least three TMC125-associated mutations were required to impair the efficacy of the drug and Y181C/V, V179F and G190S had the greatest effect on response. The prevalence of these mutations among the patients examined in our study was low. However, WGS>2 was found for one-third of our sequences. Previous nevirapine exposure was associated with an increased risk of having WGS>2 (adjusted odds ratio 1.76).

摘要

目的

评估依曲韦林(TMC125)是否对正在接受当前非核苷类逆转录酶抑制剂(NNRTIs)治疗的患者有效,我们分析了在意大利的一个大型数据库中报告的序列中 TMC125 突变的流行率以及对这种药物的基因型耐药的可能决定因素 [抗逆转录病毒耐药性队列分析(ARCA)]。

方法

我们分析了 TMC125 耐药相关突变(RAMs)的流行率和 TMC125 加权基因型评分(WGS)以及基因型耐药的决定因素。共评估了来自 2955 名 NNRTI 治疗失败患者的 5011 个序列。

结果

在 ARCA 中的序列中,68%至少有一个 TMC125 RAM,9.8%至少有三个 TMC125 RAM,而 31%的 WGS>2。常见的 RAM 是 Y181C、G190A、K101E 和 A98G,而 V179F、Y181V 和 G190S 出现在<5%的序列中。多变量分析显示,与奈韦拉平和依非韦伦暴露相关的至少三种 TMC125 RAM 的发生风险更高,而 CD4 计数>或=200 个细胞/μL 保留了其保护作用。WGS>2 的风险增加与 HIV RNA 值较高(最大值在>5 log(10) 拷贝/ml)和奈韦拉平暴露相关;CD4 计数>或=200 个细胞/μL 具有保护作用。

结论

ARCA 队列中 TMC125 耐药突变的流行率为 68%。DUET 研究表明,至少三种 TMC125 相关突变会损害药物的疗效,而 Y181C/V、V179F 和 G190S 对反应的影响最大。在我们研究中检查的患者中,这些突变的流行率较低。然而,我们的三分之一序列发现了 WGS>2。以前的奈韦拉平暴露与 WGS>2 的风险增加相关(调整后的比值比 1.76)。

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