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The trinity of the cortical actin in the initiation of HIV-1 infection.皮层肌动蛋白在 HIV-1 感染启动中的三位一体作用。
Retrovirology. 2012 May 28;9:45. doi: 10.1186/1742-4690-9-45.
3
Protein kinase C-delta regulates HIV-1 replication at an early post-entry step in macrophages.蛋白激酶 C-δ在巨噬细胞中调节 HIV-1 复制的早期进入后步骤。
Retrovirology. 2012 May 3;9:37. doi: 10.1186/1742-4690-9-37.
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Arp2/3 is critical for lamellipodia and response to extracellular matrix cues but is dispensable for chemotaxis.Arp2/3 对于片状伪足和对细胞外基质线索的反应至关重要,但对于趋化性是可有可无的。
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Actin filament attachments for sustained motility in vitro are maintained by filament bundling.肌动蛋白丝的附着对于体外的持续运动是通过丝束的捆绑来维持的。
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Viruses. 2011 Sep;3(9):1757-76. doi: 10.3390/v3091757. Epub 2011 Sep 15.
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8
Urokinase plasminogen activator inhibits HIV virion release from macrophage-differentiated chronically infected cells via activation of RhoA and PKCε.尿激酶型纤溶酶原激活物通过激活 RhoA 和 PKCε 抑制巨噬细胞分化的慢性感染细胞中 HIV 病毒粒子的释放。
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9
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10
LIM kinase 1 modulates cortical actin and CXCR4 cycling and is activated by HIV-1 to initiate viral infection.LIM 激酶 1 调节皮质肌动蛋白和 CXCR4 的循环,并且被 HIV-1 激活以启动病毒感染。
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HIV-1 触发原代 CD4 T 细胞和巨噬细胞中 WAVE2 的磷酸化,介导 Arp2/3 依赖性核迁移。

HIV-1 triggers WAVE2 phosphorylation in primary CD4 T cells and macrophages, mediating Arp2/3-dependent nuclear migration.

机构信息

National Center for Biodefense and Infectious Diseases, Department of Molecular and Microbiology, George Mason University, Manassas, Virginia 20110.

Key Laboratory of Immunology of AIDS, Ministry of Health, the First Affiliated Hospital, China Medical University, Shenyang, Liaoning province 110001, China.

出版信息

J Biol Chem. 2014 Mar 7;289(10):6949-6959. doi: 10.1074/jbc.M113.492132. Epub 2014 Jan 10.

DOI:10.1074/jbc.M113.492132
PMID:24415754
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3945356/
Abstract

The human immunodeficiency virus type 1 (HIV-1) initiates receptor signaling and early actin dynamics during viral entry. This process is required for viral infection of primary targets such as resting CD4 T cells. WAVE2 is a component of a multiprotein complex linking receptor signaling to dynamic remodeling of the actin cytoskeleton. WAVE2 directly activates Arp2/3, leading to actin nucleation and filament branching. Although several bacterial and viral pathogens target Arp2/3 for intracellular mobility, it remains unknown whether HIV-1 actively modulates the Arp2/3 complex through virus-mediated receptor signal transduction. Here we report that HIV-1 triggers WAVE2 phosphorylation at serine 351 through gp120 binding to the chemokine coreceptor CXCR4 or CCR5 during entry. This phosphorylation event involves both Gαi-dependent and -independent pathways, and is conserved both in X4 and R5 viral infection of resting CD4 T cells and primary macrophages. We further demonstrate that inhibition of WAVE2-mediated Arp2/3 activity through stable shRNA knockdown of Arp3 dramatically diminished HIV-1 infection of CD4 T cells, preventing viral nuclear migration. Inhibition of Arp2/3 through a specific inhibitor, CK548, also drastically inhibited HIV-1 nuclear migration and infection of CD4 T cells. Our results suggest that Arp2/3 and the upstream regulator, WAVE2, are essential co-factors hijacked by HIV for intracellular migration, and may serve as novel targets to prevent HIV transmission.

摘要

人类免疫缺陷病毒 1 型(HIV-1)在病毒进入时启动受体信号转导和早期肌动蛋白动力学。这一过程对于 HIV 感染静止 CD4 T 细胞等原发性靶细胞是必需的。WAVE2 是一种将受体信号转导与肌动蛋白细胞骨架动态重塑连接起来的多蛋白复合物的组成部分。WAVE2 直接激活 Arp2/3,导致肌动蛋白成核和丝状分支。尽管几种细菌和病毒病原体通过病毒介导的受体信号转导将 Arp2/3 作为细胞内迁移的靶点,但 HIV-1 是否主动通过病毒介导的受体信号转导来调节 Arp2/3 复合物仍不清楚。在这里,我们报告 HIV-1 通过 gp120 与趋化因子共受体 CXCR4 或 CCR5 结合,在进入时触发 WAVE2 在丝氨酸 351 上的磷酸化。该磷酸化事件涉及 Gαi 依赖性和非依赖性途径,并且在静止 CD4 T 细胞和原代巨噬细胞中 X4 和 R5 病毒感染中均保守。我们进一步证明,通过稳定 shRNA 敲低 Arp3 抑制 WAVE2 介导的 Arp2/3 活性,可显著降低 HIV-1 对 CD4 T 细胞的感染,阻止病毒核迁移。通过特异性抑制剂 CK548 抑制 Arp2/3 也极大地抑制了 HIV-1 的核迁移和 CD4 T 细胞的感染。我们的研究结果表明,Arp2/3 和上游调节因子 WAVE2 是 HIV 用于细胞内迁移的必需辅助因子,可能成为预防 HIV 传播的新靶点。