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首页> 外文期刊>Journal of Medical Virology >Rilpivirine resistance and the dangerous liaisons with substitutions at position 184 among patients infected with HIV-1: Analysis from a national drug-resistance database (ARCA)
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Rilpivirine resistance and the dangerous liaisons with substitutions at position 184 among patients infected with HIV-1: Analysis from a national drug-resistance database (ARCA)

机译:感染HIV-1的患者中的Rilpivirine耐药性和危险联系(第184位有替代物):来自国家耐药数据库(ARCA)的分析

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摘要

Rilpivirine (RPV) is a novel NNRTI with a mutational pattern different from first-generation drugs of the same class: 16 resistance-associated mutations (RAM) are listed, but the combination E138K+M184I seems to be the most important. Aims of the present study were to evaluate the prevalence of these RAMs in Italian HIV-1 infected patients and to assess if previous drug history could represent a risk to develop RPV-related RAMs. The analysis was performed using the ARCA database, which contains data on resistance and therapy from subjects throughout Italy. Prevalence of RPV-associated and first-generation NNRTI-associated RAMs was evaluated. Linear regression model, odds ratio and 95% Confidence Interval were used to assess factors associated with the development of RPV RAMs, substitutions at position 184 and their combinations. A total of 8,067 tests were selected within the database. In Italian HIV-positive HAART-na?ve patients, prevalence of the main RAMs for RPV is low except for E138A (present in 5.1% of subjects). The combination E138K+M184I is absent in both na?ve and experienced subjects. A previous exposure to NVP might increase the risk to develop RPV-associated RAMs. TDF, EFV, and possibly FTC may predispose to the selection for M184I. Among Italian patients the susceptibility to RPV is widespread since some severe substitutions (e.g., E138K are rare), whereas issues exist for others (i.e., E138A, Y181C) which are more frequent. Appropriate use of RPV within a therapeutic sequencing might be controversial.
机译:Rilpivirine(RPV)是一种新颖的NNRTI,其突变模式不同于同类的第一代药物:列出了16种耐药相关突变(RAM),但E138K + M184I组合似乎是最重要的。本研究的目的是评估这些RAM在意大利HIV-1感染患者中的患病率,并评估以前的药物史是否可能代表发展RPV相关RAM的风险。使用ARCA数据库进行了分析,该数据库包含来自意大利各地受试者的耐药性和治疗数据。评估了RPV相关和第一代NNRTI相关RAM的发生率。线性回归模型,比值比和95%置信区间用于评估与RPV RAM的发展,位置184处的取代及其组合相关的因素。数据库中总共选择了8067个测试。在意大利的HIV阳性HAART初治患者中,除E138A外,主要RAM的RPV患病率较低(占受试者的5.1%)。幼稚和经验丰富的受试者都没有E138K + M184I的组合。以前接触过NVP可能会增加开发与RPV相关的RAM的风险。 TDF,EFV以及可能的FTC可能会为M184I的选择提供便利。在意大利患者中,由于一些严重的替代(例如,E138K很少见),对RPV的易感性很普遍,而其他患者(例如,E138A,Y181C)则更常见。在治疗性测序中正确使用RPV可能会引起争议。

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