Cyclophilin A facilitates HIV-1 integration.

IF 4 2区 医学 Q2 VIROLOGY Journal of Virology Pub Date : 2024-11-19 Epub Date: 2024-10-31 DOI:10.1128/jvi.00947-24
Adrian Padron, Richa Dwivedi, Rajasree Chakraborty, Prem Prakash, Kyusik Kim, Jiong Shi, Jinwoo Ahn, Jui Pandhare, Jeremy Luban, Christopher Aiken, Muthukumar Balasubramaniam, Chandravanu Dash
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Abstract

Cyclophilin A (CypA) binds to the HIV-1 capsid to facilitate reverse transcription and nuclear entry and counter the antiviral activity of TRIM5α. Interestingly, recent studies suggest that the capsid enters the nucleus of an infected cell and uncoats prior to integration. We have previously reported that the capsid protein regulates HIV-1 integration. Therefore, we probed whether CypA-capsid interaction also regulates this post-nuclear entry step. First, we challenged CypA-expressing (CypA+/+) and CypA-depleted (CypA-/-) cells with HIV-1 and quantified the levels of provirus. CypA-depletion significantly reduced integration, an effect that was independent of CypA's effect on reverse transcription, nuclear entry, and the presence or absence of TRIM5α. In addition, cyclosporin A, an inhibitor that disrupts CypA-capsid binding, inhibited proviral integration in CypA+/+ cells but not in CypA-/- cells. HIV-1 capsid mutants (G89V and P90A) deficient in CypA binding were also blocked at the integration step in CypA+/+ cells but not in CypA-/- cells. Then, to understand the mechanism, we assessed the integration activity of the HIV-1 preintegration complexes (PICs) extracted from acutely infected cells. PICs from CypA-/- cells retained lower integration activity in vitro compared to those from CypA+/+ cells. PICs from cells depleted of both CypA and TRIM5α also had lower activity, suggesting that CypA's effect on PIC was independent of TRIM5α. Finally, CypA protein specifically stimulated PIC activity, as this effect was significantly blocked by CsA. Collectively, these results provide strong evidence that CypA directly promotes HIV-1 integration, a previously unknown role of this host factor in the nucleus of an infected cell.

Importance: Interaction between the HIV-1 capsid and host cellular factors is essential for infection. However, the molecular details and functional consequences of viral-host factor interactions during HIV-1 infection are not fully understood. Over 30 years ago, Cyclophilin A (CypA) was identified as the first host protein to bind to the HIV-1 capsid. Now it is established that CypA-capsid interaction promotes reverse transcription and nuclear entry of HIV-1. In addition, CypA blocks TRIM5α-mediated restriction of HIV-1. In this report, we show that CypA promotes the post-nuclear entry step of HIV-1 integration by binding to the viral capsid. Notably, we show that CypA stimulates the viral DNA integration activity of the HIV-1 preintegration complex. Collectively, our studies identify a novel role of CypA during the early steps of HIV-1 infection. This new knowledge is important because recent reports suggest that an operationally intact HIV-1 capsid enters the nucleus of an infected cell.

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Cyclophilin A 可促进 HIV-1 整合。
嗜环蛋白 A(CypA)与 HIV-1 的外壳结合,促进逆转录和进入细胞核,并对抗 TRIM5α 的抗病毒活性。有趣的是,最近的研究表明,噬菌体进入受感染细胞的细胞核,并在整合前脱衣。我们以前曾报道过,噬菌体蛋白能调节 HIV-1 的整合。因此,我们探究了 CypA 与噬菌体的相互作用是否也调控这一进入细胞核后的步骤。首先,我们用HIV-1挑战了CypA表达(CypA+/+)和CypA缺失(CypA-/-)细胞,并量化了前病毒的水平。CypA缺失大大降低了整合,这种效应与CypA对反转录、核进入以及TRIM5α存在与否的影响无关。此外,环孢素 A(一种能破坏 CypA 与噬菌体结合的抑制剂)能抑制 CypA+/+ 细胞中的病毒整合,但不能抑制 CypA-/- 细胞中的病毒整合。缺乏CypA结合的HIV-1噬菌体突变体(G89V和P90A)在CypA+/+细胞中也会被阻断整合步骤,但在CypA-/-细胞中不会。然后,为了了解其机制,我们评估了从急性感染细胞中提取的 HIV-1 整合前复合物(PICs)的整合活性。与来自 CypA+/+ 细胞的 PICs 相比,来自 CypA-/- 细胞的 PICs 在体外保持较低的整合活性。同时去除了 CypA 和 TRIM5α 的细胞的 PIC 活性也较低,这表明 CypA 对 PIC 的影响与 TRIM5α 无关。最后,CypA 蛋白能特异性地刺激 PIC 的活性,因为 CsA 能显著阻断这种作用。总之,这些结果提供了强有力的证据,证明 CypA 直接促进了 HIV-1 的整合,而这种宿主因子在受感染细胞核中的作用以前是未知的:HIV-1外壳与宿主细胞因子之间的相互作用对感染至关重要。然而,人们对 HIV-1 感染过程中病毒-宿主因子相互作用的分子细节和功能后果还不完全了解。30 多年前,Cyclophilin A(CypA)被确定为第一个与 HIV-1 荚膜结合的宿主蛋白。现在已经确定,CypA-capsid 相互作用促进了 HIV-1 的逆转录和核进入。此外,CypA 还能阻止 TRIM5α 介导的 HIV-1 限制。在本报告中,我们发现 CypA 通过与病毒外壳结合,促进了 HIV-1 整合的核进入后步骤。值得注意的是,我们发现 CypA 能刺激 HIV-1 整合前复合体的病毒 DNA 整合活性。总之,我们的研究发现了 CypA 在 HIV-1 感染早期阶段的新作用。这一新的知识非常重要,因为最近的报道表明,完整的 HIV-1 荚膜会进入受感染细胞的细胞核。
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来源期刊
Journal of Virology
Journal of Virology 医学-病毒学
CiteScore
10.10
自引率
7.40%
发文量
906
审稿时长
1 months
期刊介绍: Journal of Virology (JVI) explores the nature of the viruses of animals, archaea, bacteria, fungi, plants, and protozoa. We welcome papers on virion structure and assembly, viral genome replication and regulation of gene expression, genetic diversity and evolution, virus-cell interactions, cellular responses to infection, transformation and oncogenesis, gene delivery, viral pathogenesis and immunity, and vaccines and antiviral agents.
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