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Significance of amino acid variation at human immunodeficiency virus type 1 reverse transcriptase residue 210 for zidovudine susceptibility.

机译:氨基酸变异在人免疫缺陷病毒1型逆转录酶残基210对齐多夫定敏感性的影响。

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摘要

Amino acid variation at reverse transcriptase (RT) codon 210 (generally Leu-210 to Trp [L210W], TTG-->TGG) is occasionally detected after the initiation of azidothymidine (AZT) therapy. The impact of this variation on AZT resistance and viral replication was addressed by four different approaches. The frequency and genetic background of the L210W mutation in vivo were assessed by analyzing sera of AZT-naive and AZT-experienced patients by RT-PCR and DNA sequencing. The degree of AZT resistance (50% infective concentration [IC50]) of recombinant viruses constructed by using the RT of 21 clinical isolates was stratified by the presence or absence of the 210 mutation. The AZT IC50S of a panel of mutant viruses (with or without W-210) constructed by site-directed mutagenesis in an HXB2 background were assayed by using a HeLa CD4 plaque reduction assay. Finally, the effect of the 210 mutation on viral replication was assessed by replication competition of an AZT-resistant virus, RTMN (L-41/Y-215), and RTMN with the W-210 mutation in the presence and in the absence of AZT. In AZT-naive patients, tryptophan at RT residue 210 was rare. After AZT exposure, W-210 appeared in a minority of those patients, most commonly in association with L-41 and Y-215. The presence of W-210 increased the AZTIC50 by two- to fourfold, as determined by both the recombinant virus assay and site-directed mutagenesis. A significant replication advantage in favor of the wild-type L-210 over W-210 was observed, although the selection against the 210 mutant was two- to threefold lower when the viruses were grown in the presence of 5 microM AZT. In summary, the L210W mutation appears to be of marginal significance, conferring approximately two- to fourfold-reduced sensitivity to AZT compared with similar AZT-resistant genomes with L-210. The selection pressure against W-210 may account for the modest proportion of patients in which W-210 appears in vivo.
机译:启动叠氮胸苷(AZT)治疗后,偶尔会检测到逆转录酶(RT)210密码子(通常是Leu-210至Trp [L210W],TTG→TGG)的氨基酸变化。通过四种不同的方法解决了这种变异对AZT耐药性和病毒复制的影响。体内L210W突变的频率和遗传背景是通过RT-PCR和DNA测序分析未经AZT感染和有AZT经验的患者的血清来评估的。使用21种临床分离株的RT构建的重组病毒的AZT抗性程度(50%感染浓度[IC50])通过210突变的存在与否进行分层。通过使用HeLa CD4噬菌斑减少测定法,通过在HXB2背景中进行定点诱变构建了一组突变病毒(有或没有W-210)的AZT IC50S。最后,通过存在和不存在W-210突变的AZT抗性病毒,RTMN(L-41 / Y-215)和带有W-210突变的RTMN的复制竞争,评估210突变对病毒复制的影响。 AZT。在未经AZT治疗的患者中,RT残基210处的色氨酸很少见。 AZT暴露后,少数患者出现了W-210,最常见的是与L-41和Y-215相关。 W-210的存在使AZTIC50增加了2到4倍,这是通过重组病毒测定和定点诱变确定的。尽管当病毒在5 microM AZT存在下生长时,针对210突变体的选择降低了2至3倍,但观察到比W-210具有明显的有利于野生型L-210的复制优势。总而言之,与具有L-210的类似AZT耐药基因组相比,L210W突变似乎具有很小的意义,对AZT的敏感性降低了约2到4倍。针对W-210的选择压力可能解释了体内出现W-210的患者的适度比例。

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