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Nevirapine-resistant human immunodeficiency virus: kinetics of replication and estimated prevalence in untreated patients.

机译:耐奈韦拉平的人类免疫缺陷病毒:未经治疗的患者的复制动力学和估计患病率。

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摘要

The nonnucleoside reverse transcriptase inhibitor nevirapine rapidly selects for mutant human immunodeficiency virus (HIV) in vivo. The most common mutation occurs at amino acid residue 181 in patients receiving monotherapy. After the initiation of nevirapine therapy, plasma and peripheral blood mononuclear cell samples were collected at frequent intervals and assayed for HIV RNA levels and the proportion of virus containing a mutation at residue 181. HIV RNA levels remained stable for the first 24 h after initiation of therapy and rapidly declined between 1 and 7 days. There was a consistent maximum decrease of 2 log10 HIV RNA copies per ml of plasma (range, 1.96 to 2.43) from baseline after 2 weeks in all monotherapy subjects. The estimated median half-life of HIV RNA was 1.11 days (range, 0.63 to 1.61). After 14 days of therapy, HIV RNA levels began to increase and 181 mutant virus was detected. The estimated doubling time of the emerging virus population ranged from 1.80 to 5.73 days. Viral DNA in peripheral blood mononuclear cells turned over from wild type to the mutant with a mutation at residue 181 significantly more slowly than did HIV RNA in plasma. In two subjects, the calculated prevalence of the 181 mutant virus prior to treatment was 7 and 133 per 10,000 copies of plasma HIV RNA.
机译:非核苷逆转录酶抑制剂奈韦拉平可在体内快速选择突变型人免疫缺陷病毒(HIV)。在接受单一疗法的患者中,最常见的突变发生在氨基酸残基181处。开始使用奈韦拉平治疗后,应定期采集血浆和外周血单个核细胞样品,并检测HIV RNA水平以及在第181位残基处含有突变的病毒的比例。治疗后1到7天迅速下降。在所有单药治疗受试者中,均在2周后每毫升血浆中出现2个log10 HIV RNA拷贝持续不断地最大减少(从1.96到2.43),从基线开始。 HIV RNA的估计中值半衰期为1.11天(范围为0.63至1.61)。经过14天的治疗,HIV RNA水平开始升高,并检测到181种突变病毒。估计新兴病毒种群的倍增时间为1.80至5.73天。与血浆中的HIV RNA相比,外周血单核细胞中的病毒DNA从野生型转变为具有181位残基突变的突变体的速度要慢得多。在两名受试者中,治疗前181种突变病毒的计算患病率是每10,000个血浆HIV RNA分别为7和133。

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