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逆转录病毒多蛋白晶体结构:泡沫病毒蛋白酶-逆转录酶(PR-RT)原型。

Crystal Structure of a Retroviral Polyprotein: Prototype Foamy Virus Protease-Reverse Transcriptase (PR-RT).

机构信息

Center for Advanced Biotechnology and Medicine (CABM), Rutgers University, Piscataway, NJ 08854, USA.

Department of Medicinal Chemistry, Ernest Mario School of Pharmacy, Rutgers University, Piscataway, NJ 08854, USA.

出版信息

Viruses. 2021 Jul 29;13(8):1495. doi: 10.3390/v13081495.

Abstract

In most cases, proteolytic processing of the retroviral Pol portion of the Gag-Pol polyprotein precursor produces protease (PR), reverse transcriptase (RT), and integrase (IN). However, foamy viruses (FVs) express Pol separately from Gag and, when Pol is processed, only the IN domain is released. Here, we report a 2.9 Å resolution crystal structure of the mature PR-RT from prototype FV (PFV) that can carry out both proteolytic processing and reverse transcription but is in a configuration not competent for proteolytic or polymerase activity. PFV PR-RT is monomeric and the architecture of PFV PR is similar to one of the subunits of HIV-1 PR, which is a dimer. There is a C-terminal extension of PFV PR (101-145) that consists of two helices which are adjacent to the base of the RT palm subdomain, and anchors PR to RT. The polymerase domain of PFV RT consists of fingers, palm, thumb, and connection subdomains whose spatial arrangements are similar to the p51 subunit of HIV-1 RT. The RNase H and polymerase domains of PFV RT are connected by flexible linkers. Significant spatial and conformational (sub)domain rearrangements are therefore required for nucleic acid binding. The structure of PFV PR-RT provides insights into the conformational maturation of retroviral Pol polyproteins.

摘要

在大多数情况下,逆转录病毒 Pol 部分的蛋白水解加工会产生蛋白酶(PR)、逆转录酶(RT)和整合酶(IN)。然而,泡沫病毒(FVs)将 Pol 与 Gag 分开表达,当 Pol 被加工时,只有 IN 结构域被释放。在这里,我们报告了一个 2.9 Å 分辨率的原型 FV(PFV)成熟 PR-RT 的晶体结构,它可以进行蛋白水解加工和逆转录,但不具备蛋白水解或聚合酶活性。PFV PR-RT 是单体的,PFV PR 的结构类似于 HIV-1 PR 的一个亚基,HIV-1 PR 是二聚体。PFV PR 有一个 C 端延伸(101-145),由两个螺旋组成,它们与 RT 手掌亚基的底部相邻,并将 PR 锚定在 RT 上。PFV RT 的聚合酶结构域由手指、手掌、拇指和连接亚基组成,其空间排列与 HIV-1 RT 的 p51 亚基相似。PFV RT 的 RNase H 和聚合酶结构域由柔性接头连接。因此,需要进行显著的空间和构象(亚)域重排才能结合核酸。PFV PR-RT 的结构为逆转录病毒 Pol 多蛋白的构象成熟提供了深入的了解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6f31/8402755/2483333b593a/viruses-13-01495-g001.jpg

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