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Construction of a Human Immunodeficiency Virus Type 1 (HIV-1) Library Containing Random Combinations of Amino Acid Substitutions in the HIV-1 Protease due to Resistance by Protease Inhibitors

机译:人免疫缺陷病毒1型(HIV-1)文库的构建,该文库因蛋白酶抑制剂的抗性而在HIV-1蛋白酶中包含氨基酸取代的随机组合。

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摘要

Human immunodeficiency virus type 1 (HIV-1) heterogeneity contributes to the emergence of drug-resistant virus, escape from host defense systems, and/or conversion of the cellular tropism. To establish an in vitro system to address a heterogeneous virus population, we constructed a library of HIV-1 molecular clones containing a set of random combinations of zero to 11 amino acid substitutions associated with resistance to protease inhibitors by the HIV-1 protease. The complexity (2.1 × 105) of the HIV-1 library pNG-PRL was large enough to cover all of the possible combinations of zero to 11 amino acid substitutions (a total of 4,096 substitutions possible). The T-cell line MT-2 was infected with the HIV-1 library, and resistant viruses were selected after treatment by the protease inhibitor ritonavir (0.03 to 0.30 μM). The viruses that contained three to eight amino acid substitutions could be selected within 2 weeks. These results demonstrate that this HIV-1 library could serve as an alternative in vitro system to analyze the emergence of drug resistance and to evaluate the antiviral activity of novel compounds against multidrug-resistant viruses.
机译:人类1型免疫缺陷病毒(HIV-1)的异质性有助于耐药性病毒的出现,从宿主防御系统逃逸和/或细胞向性转化。为了建立一个针对异种病毒种群的体外系统,我们构建了一个HIV-1分子克隆文库,该文库包含一组零到11个氨基酸取代的随机组合,与HIV-1蛋白酶对蛋白酶抑制剂的抗性相关。 HIV-1文库pNG-PRL的复杂度(2.1×105)足够大,可以覆盖从0到11个氨基酸取代的所有可能组合(总共4,096个取代)。 T细胞系MT-2感染了HIV-1文库,经蛋白酶抑制剂利托那韦(0.03至0.30μM)处理后,选择了抗性病毒。可以在2周内选择包含3至8个氨基酸取代的病毒。这些结果表明,该HIV-1文库可以用作替代的体外系统,以分析耐药性的出现并评估新型化合物对耐多药病毒的抗病毒活性。

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