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在接受结构化治疗中断的受试者中出现携带M184V和L90M突变的少量1型人类免疫缺陷病毒群体。

Emergence of minor populations of human immunodeficiency virus type 1 carrying the M184V and L90M mutations in subjects undergoing structured treatment interruptions.

作者信息

Metzner Karin J, Bonhoeffer Sebastian, Fischer Marek, Karanicolas Rose, Allers Kristina, Joos Beda, Weber Rainer, Hirschel Bernard, Kostrikis Leondios G, Günthard Huldrych F

机构信息

Aaron Diamond AIDS Research Center, Columbia University, New York, New York, USA.

出版信息

J Infect Dis. 2003 Nov 15;188(10):1433-43. doi: 10.1086/379215. Epub 2003 Nov 3.

Abstract

The use of structured treatment interruption (STI) in human immunodeficiency virus (HIV)-infected subjects is currently being studied as an alternative therapeutic strategy for HIV-1. The potential risk for selection of drug-resistant HIV-1 variants during STI is unknown and remains a concern. Therefore, the emergence of drug resistance in sequential plasma samples obtained from 28 subjects with chronic HIV infection was studied. They underwent 4 cycles of 2-week STI, followed by 8-week retreatment with highly active antiretroviral therapy identical to that used before STI, and they had never failed treatment before undergoing STI. At week 40, treatment was stopped for a longer period. Minor populations of drug-resistant variants were detected by quantitative real-time polymerase chain reaction, by use of allele-discriminating oligonucleotides for 2 key resistance mutations: L90M (protease) and M184V (reverse transcriptase). The approximate discriminative power was 0.1%. In 14 of 25 and in 3 of 25 subjects, the M184V and the L90M mutations, respectively, were detected as minor populations, at different times during STI. Overall, these results indicate that, in subjects undergoing multiple STIs, HIV-1 variants carrying drug-resistance mutations can emerge during periods of increased HIV-1 replication.

摘要

目前正在研究在人类免疫缺陷病毒(HIV)感染受试者中使用结构化治疗中断(STI)作为HIV-1的一种替代治疗策略。STI期间选择耐药HIV-1变异体的潜在风险尚不清楚,仍是一个令人担忧的问题。因此,对28例慢性HIV感染受试者连续血浆样本中耐药性的出现情况进行了研究。他们接受了4个周期的为期2周的STI,随后用与STI前相同的高效抗逆转录病毒疗法进行为期8周的再治疗,并且在接受STI之前他们从未治疗失败过。在第40周时,治疗停止更长时间。通过定量实时聚合酶链反应,使用针对2个关键耐药突变(L90M(蛋白酶)和M184V(逆转录酶))的等位基因鉴别寡核苷酸,检测到耐药变异体的少数群体。近似鉴别力为0.1%。在25名受试者中的14名以及25名受试者中的3名中,分别在STI期间的不同时间检测到M184V和L90M突变作为少数群体。总体而言,这些结果表明,在接受多次STI的受试者中,携带耐药突变的HIV-1变异体可在HIV-1复制增加期间出现。

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