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Functional complementation of nucleocapsid and late domain PTAP mutants of human immunodeficiency virus type 1 during replication.

机译:复制过程中人免疫缺陷病毒1型的核衣壳和晚期结构域PTAP突变体的功能互补。

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During human immunodeficiency virus type 1 (HIV-1) assembly, the nucleocapsid (NC) and the PTAP motif in p6 of Gag play important roles in RNA encapsidation and virus release, respectively. We have previously demonstrated that functional complementation occurs between an NC mutant and a PTAP mutant to rescue viral replication. In this report, we examined the amounts of functional NC and PTAP motif that are required during virus replication. When NC and PTAP mutants were coexpressed at 5:1, 5:5, and 1:5 ratios, virus titers were rescued at 5%, 51%, and 86% of the wild-type level, respectively. These results indicate that HIV-1 requires a small amount of functional PTAP motif but far more functional NC to complete efficient replication. Further analyses reveal that RNA packaging can be significantly rescued in viruses containing a small amount of functional NC. However, most of the NC proteins must be functional to generate the wild-type level of R-U5 DNA product. Once the R-U5 product is generated, viruses containing half of the functional NC can complete reverse transcription and DNA integration at near-wild-type efficiency. These results define the quantitative requirements of NC and p6 during HIV-1 replication and provide insights into the requirement for the development of anti-HIV strategies using NC and p6 as targets.
机译:在人类1型免疫缺陷病毒(HIV-1)组装过程中,Gag p6中的核衣壳(NC)和PTAP图案分别在RNA衣壳化和病毒释放中发挥重要作用。我们以前已经证明,在NC突变体和PTAP突变体之间发生功能互补,以抢救病毒复制。在此报告中,我们检查了病毒复制过程中所需的功能性NC和PTAP基序的数量。当NC和PTAP突变体以5:1、5:5和1:5的比率共表达时,病毒滴度分别以野生型水平的5%,51%和86%拯救。这些结果表明,HIV-1需要少量的功能性PTAP基序,而功能性NC则要多得多,才能完成有效的复制。进一步的分析表明,在含有少量功能性NC的病毒中,RNA包装可以得到显着拯救。但是,大多数NC蛋白必​​须具有产生野生型R-U5 DNA产物的功能。一旦生成R-U5产品,包含一半功能性NC的病毒就可以以接近野生型的效率完成逆转录和DNA整合。这些结果确定了在HIV-1复制过程中NC和p6的定量要求,并提供了以NC和p6为目标制定抗HIV策略的要求的见解。

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