在自然疾病抗性宿主与非自然疾病易感性宿主的 CD4+T 细胞中，由 SIV 复制所掺入的不同宿主细胞蛋白。

Distinct host cell proteins incorporated by SIV replicating in CD4+ T cells from natural disease resistant versus non-natural disease susceptible hosts.

机构信息

Department of Pathology & Laboratory Medicine, Emory University School of Medicine, Atlanta, GA 30322, USA.

出版信息

Retrovirology. 2010 Dec 16;7:107. doi: 10.1186/1742-4690-7-107.

DOI:10.1186/1742-4690-7-107

PMID:21162735

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3012658/

Abstract

BACKGROUND

Enveloped viruses including the simian immunodeficiency virus (SIV) replicating within host cells acquire host proteins upon egress from the host cells. A number of studies have catalogued such host proteins, and a few have documented the potential positive and negative biological functions of such host proteins. The studies conducted herein utilized proteomic analysis to identify differences in the spectrum of host proteins acquired by a single source of SIV replicating within CD4+ T cells from disease resistant sooty mangabeys and disease susceptible rhesus macaques.

RESULTS

While a total of 202 host derived proteins were present in viral preparations from CD4+ T cells from both species, there were 4 host-derived proteins that consistently and uniquely associated with SIV replicating within CD4+ T cells from rhesus macaques but not sooty mangabeys; and, similarly, 28 host-derived proteins that uniquely associated with SIV replicating within CD4+ T cells from sooty mangabeys, but not rhesus macaques. Of interest was the finding that of the 4 proteins uniquely present in SIV preparations from rhesus macaques was a 26 S protease subunit 7 (MSS1) that was shown to enhance HIV-1 'tat' mediated transactivation. Among the 28 proteins found in SIV preparations from sooty mangabeys included several molecules associated with immune function such as CD2, CD3ε, TLR4, TLR9 and TNFR and a bioactive form of IL-13.

CONCLUSIONS

The finding of 4 host proteins that are uniquely associated with SIV replicating within CD4+ T cells from disease susceptible rhesus macaques and 28 host proteins that are uniquely associated with SIV replicating within CD4+ T cells from disease resistant sooty mangabeys provide the foundation for determining the potential role of each of these unique host-derived proteins in contributing to the polarized clinical outcome in these 2 species of nonhuman primates.

摘要

背景

在宿主细胞中复制的包膜病毒（包括猴免疫缺陷病毒[SIV]）在离开宿主细胞时会获得宿主蛋白。许多研究已经对这些宿主蛋白进行了编目，其中一些研究记录了这些宿主蛋白的潜在积极和消极生物学功能。本文进行的研究利用蛋白质组学分析来鉴定在抵抗疾病的黑眉长尾猴和易患疾病的恒河猴的 CD4+T 细胞中由单一来源的 SIV 复制所获得的宿主蛋白谱的差异。

结果

虽然在来自这两个物种的 CD4+T 细胞的病毒制剂中总共存在 202 种宿主来源的蛋白质，但有 4 种宿主来源的蛋白质始终与仅在恒河猴的 CD4+T 细胞中复制的 SIV 相关，而与黑眉长尾猴无关；同样，有 28 种宿主来源的蛋白质仅与黑眉长尾猴的 CD4+T 细胞中复制的 SIV 相关，而与恒河猴无关。有趣的是，在仅在恒河猴的 SIV 制剂中存在的 4 种蛋白质中，有一个 26S 蛋白酶亚基 7（MSS1），它被证明可以增强 HIV-1“tat”介导的反式激活。在黑眉长尾猴的 SIV 制剂中发现的 28 种蛋白质中，包括一些与免疫功能相关的分子，如 CD2、CD3ε、TLR4、TLR9 和 TNFR 以及具有生物活性的 IL-13。

结论

在易患疾病的恒河猴的 CD4+T 细胞中与 SIV 复制相关的 4 种宿主蛋白和在抵抗疾病的黑眉长尾猴的 CD4+T 细胞中与 SIV 复制相关的 28 种宿主蛋白的发现为确定这些独特的宿主衍生蛋白在这两个非人类灵长类物种中对极化临床结局的潜在作用提供了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d0f3/3012658/26ea58ceae53/1742-4690-7-107-1.jpg

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在自然疾病抗性宿主与非自然疾病易感性宿主的 CD4+T 细胞中，由 SIV 复制所掺入的不同宿主细胞蛋白。

Distinct host cell proteins incorporated by SIV replicating in CD4+ T cells from natural disease resistant versus non-natural disease susceptible hosts.

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背景

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