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HIV-人体蛋白质复合物的全球格局。

Global landscape of HIV-human protein complexes.

机构信息

Department of Cellular and Molecular Pharmacology, University of California, San Francisco, California 94158, USA.

出版信息

Nature. 2011 Dec 21;481(7381):365-70. doi: 10.1038/nature10719.

Abstract

Human immunodeficiency virus (HIV) has a small genome and therefore relies heavily on the host cellular machinery to replicate. Identifying which host proteins and complexes come into physical contact with the viral proteins is crucial for a comprehensive understanding of how HIV rewires the host's cellular machinery during the course of infection. Here we report the use of affinity tagging and purification mass spectrometry to determine systematically the physical interactions of all 18 HIV-1 proteins and polyproteins with host proteins in two different human cell lines (HEK293 and Jurkat). Using a quantitative scoring system that we call MiST, we identified with high confidence 497 HIV-human protein-protein interactions involving 435 individual human proteins, with ∼40% of the interactions being identified in both cell types. We found that the host proteins hijacked by HIV, especially those found interacting in both cell types, are highly conserved across primates. We uncovered a number of host complexes targeted by viral proteins, including the finding that HIV protease cleaves eIF3d, a subunit of eukaryotic translation initiation factor 3. This host protein is one of eleven identified in this analysis that act to inhibit HIV replication. This data set facilitates a more comprehensive and detailed understanding of how the host machinery is manipulated during the course of HIV infection.

摘要

人类免疫缺陷病毒 (HIV) 的基因组较小,因此严重依赖宿主细胞机制进行复制。确定哪些宿主蛋白和复合物与病毒蛋白发生物理接触对于全面了解 HIV 在感染过程中如何重编宿主细胞机制至关重要。在这里,我们报告了使用亲和标记和纯化质谱法来系统地确定两种不同的人类细胞系(HEK293 和 Jurkat)中所有 18 种 HIV-1 蛋白和多蛋白与宿主蛋白的物理相互作用。使用我们称为 MiST 的定量评分系统,我们鉴定了具有高置信度的 497 种 HIV-人类蛋白-蛋白相互作用,涉及 435 种不同的人类蛋白,其中约 40%的相互作用在两种细胞类型中都被鉴定出来。我们发现,HIV 劫持的宿主蛋白,特别是在两种细胞类型中都发现相互作用的蛋白,在灵长类动物中高度保守。我们发现了一些被病毒蛋白靶向的宿主复合物,包括 HIV 蛋白酶切割真核翻译起始因子 3 的 eIF3d 亚基的发现。在这项分析中,该宿主蛋白是被鉴定出的 11 种抑制 HIV 复制的蛋白之一。该数据集有助于更全面和详细地了解宿主机制在 HIV 感染过程中是如何被操纵的。

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