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首页> 外文期刊>Virology >IN VITRO SELECTION FOR DIFFERENT MUTATIONAL PATTERNS IN THE HIV-1 REVERSE TRANSCRIPTASE USING HIGH AND LOW SELECTIVE PRESSURE OF THE NONNUCLEOSIDE REVERSE TRANSCRIPTASE INHIBITOR HBY 097
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IN VITRO SELECTION FOR DIFFERENT MUTATIONAL PATTERNS IN THE HIV-1 REVERSE TRANSCRIPTASE USING HIGH AND LOW SELECTIVE PRESSURE OF THE NONNUCLEOSIDE REVERSE TRANSCRIPTASE INHIBITOR HBY 097

机译:使用高和低选择性的核苷类逆转录酶抑制剂HBY 097体外选择HIV-1逆转录酶中的不同突变型

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摘要

In vitro resistance of HIV-1 against high levels of HBY 097 ((S)-4-isopropoxycarbonyl-6-methoxy-3-(methylthiomethyl)-3, 4-dihydro-quinoxaline-2(1H)-thione) and other quinoxaline nonnucleoside reverse transcriptase inhibitors (NNRTIs) is characterized by a specific amino acid substitution in the reverse transcriptase (RT), Gly190Glu. This change results in decreased RT polymerase activity and in reduced growth properties of the corresponding viral variant. Here we show that the appearance of the crippling mutation at codon 190 can be prevented by lowering the selective pressure exerted by HBY 097. Under low selective pressure an accumulation of other NNRTI-specific mutations is observed. Up to five NNRTI-specific substitutions were detected in some of these virus lineages. In addition, we report novel RT amino acid changes which were not observed previously, including Val106lle, Val106Leu, and Gly190Thr. HBY 097 selects for different mutational patterns under high and low selective pressure conditions, respectively. Thus, the type of mutations which appear in HIV-infected patients undergoing therapy may be determined by the levels of the selecting drug.
机译:HIV-1对高水平HBY 097((S)-4-异丙氧基羰基-6-甲氧基-3-(甲硫基甲基)-3、4-二氢喹喔啉-2(1H)-硫酮)和其他喹喔啉的体外抗药性非核苷逆转录酶抑制剂(NNRTIs)的特征是逆转录酶(RT)Gly190Glu中有特定的氨基酸取代。该变化导致RT聚合酶活性降低和相应病毒变体的生长特性降低。在这里,我们表明可以通过降低HBY 097施加的选择压力来防止190号密码子处残缺突变的出现。在低选择压力下,观察到其他NNRTI特异性突变的积累。在其中一些病毒谱系中最多检测到五个NNRTI特异性取代。此外,我们报告了以前未观察到的新型RT氨基酸变化,包括Val106lle,Val106Leu和Gly190Thr。 HBY 097分别在高和低选择压力条件下选择不同的突变模式。因此,可以通过选择药物的水平来确定在接受治疗的HIV感染患者中出现的突变类型。

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