首页> 美国卫生研究院文献>Journal of Virology >Cyclophilin A is required for the replication of group M human immunodeficiency virus type 1 (HIV-1) and simian immunodeficiency virus SIV(CPZ)GAB but not group O HIV-1 or other primate immunodeficiency viruses.
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Cyclophilin A is required for the replication of group M human immunodeficiency virus type 1 (HIV-1) and simian immunodeficiency virus SIV(CPZ)GAB but not group O HIV-1 or other primate immunodeficiency viruses.

机译:复制M型人类免疫缺陷病毒1型(HIV-1)和猿猴免疫缺陷病毒SIV(CPZ)GAB时需要亲环蛋白A但复制O型HIV-1或其他灵长类动物免疫缺陷病毒则不需要。

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摘要

The human immunodeficiency virus type 1 (HIV-1) Gag polyprotein binds to cyclophilin A and incorporates this cellular peptidyl prolyl-isomerase into virions. Disruption of cyclophilin A incorporation, either by gag mutations or by cyclosporine A, inhibits virion infectivity, indicating that cyclophilin A plays an essential role in the HIV-1 life cycle. Using assays for packaging of cyclophilin A into virions and for viral replication sensitivity to cyclosporine A, as well as information gleaned from the alignment of Gag residues encoded by representative viral isolates, we demonstrate that of the five lineages of primate immunodeficiency viruses, only HIV-1 requires cyclophilin A for replication. Cloned viral isolates from clades A, B, and D of HIV-1 group M, as well as a phylogenetically related isolate from chimpanzee, all require cyclophilin A for replication. In contrast, the replication of two outlier (group O) HIV-1 isolates is unaffected by concentrations of cyclosporine A which disrupt cyclophilin A incorporation into virions, indicating that these viruses are capable of replicating independently of cyclophilin A. These studies identify the first phenotypic difference between HIV-1 group M and group O and are consistent with phylogenetic studies suggesting that the two HIV-1 groups were introduced into human populations via separate zoonotic transmission events.
机译:1型人类免疫缺陷病毒(HIV-1)Gag多蛋白与亲环蛋白A结合,并将这种细胞肽基脯氨酰异构酶整合到病毒体中。通过gag突变或环孢菌素A破坏亲环素A掺入会抑制病毒体感染性,这表明亲环素A在HIV-1生命周期中起着至关重要的作用。通过使用将亲环蛋白A包装到病毒颗粒中以及对环孢菌素A进行病毒复制敏感性分析以及从代表性病毒分离株编码的Gag残基比对中收集的信息,我们证明了灵长类免疫缺陷病毒的五种谱系中,只有HIV- 1需要亲环蛋白A进行复制。来自HIV-1组M进化枝A,B和D的克隆病毒分离株,以及来自黑猩猩的系统发育相关分离株,都需要亲环蛋白A才能复制。相反,两个异常(O型)HIV-1分离株的复制不受环孢菌素A浓度的影响,该浓度会破坏亲环蛋白A掺入病毒颗粒,表明这些病毒能够独立于亲环蛋白A复制。这些研究确定了第一个表型HIV-1组M和O组之间的差异,并且与系统发育研究一致,表明这两个HIV-1组是通过单独的人畜共患病传播事件引入人类的。

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