定量蛋白质组学分析 HIV-1 感染的 CD4+T 细胞揭示了重要生物学途径中的早期宿主反应:蛋白质合成、细胞增殖和 T 细胞激活。
Quantitative proteomic analysis of HIV-1 infected CD4+ T cells reveals an early host response in important biological pathways: protein synthesis, cell proliferation, and T-cell activation.
机构信息
Department of Microbiology, University of Washington, Seattle, WA 98195-8070, USA.
出版信息
Virology. 2012 Jul 20;429(1):37-46. doi: 10.1016/j.virol.2012.03.026. Epub 2012 Apr 26.
Abstract
Human immunodeficiency virus (HIV-1) depends upon host-encoded proteins to facilitate its replication while at the same time inhibiting critical components of innate and/or intrinsic immune response pathways. To characterize the host cell response on protein levels in CD4+ lymphoblastoid SUP-T1 cells after infection with HIV-1 strain LAI, we used mass spectrometry (MS)-based global quantitation with iTRAQ (isobaric tag for relative and absolute quantification). We found 266, 60 and 22 proteins differentially expressed (DE) (P-value ≤ 0.05) at 4, 8, and 20 hours post-infection (hpi), respectively, compared to time-matched mock-infected samples. The majority of changes in protein abundance occurred at an early stage of infection well before the de novo production of viral proteins. Functional analyses of these DE proteins showed enrichment in several biological pathways including protein synthesis, cell proliferation, and T-cell activation. Importantly, these early changes before the time of robust viral production have not been described before.
摘要
人类免疫缺陷病毒(HIV-1)依赖宿主编码的蛋白来促进其复制,同时抑制先天和/或固有免疫反应途径的关键成分。为了在感染 HIV-1 株 LAI 后在 CD4+淋巴母细胞系 SUP-T1 细胞的蛋白质水平上描述宿主细胞反应,我们使用基于质谱(MS)的 iTRAQ(相对和绝对定量的同重同位素标记)进行全局定量。与时间匹配的 mock 感染样本相比,我们分别在感染后 4、8 和 20 小时(hpi)发现了 266、60 和 22 个差异表达(DE)的蛋白(P 值≤0.05)。蛋白丰度的大多数变化发生在感染的早期阶段,远在病毒蛋白从头合成之前。对这些 DE 蛋白的功能分析表明,它们在包括蛋白质合成、细胞增殖和 T 细胞激活在内的几个生物学途径中富集。重要的是,在强大的病毒产生之前,这些早期变化以前没有被描述过。
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