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利用无偏蛋白质组学分析理解人巨细胞病毒潜伏感染

Understanding HCMV Latency Using Unbiased Proteomic Analyses.

作者信息

Poole Emma, Sinclair John

机构信息

Department of Medicine, University of Cambridge, box 157, Level 5 Addenbrooke's Hospital, Hills Road, Cambridge CB2 0QQ, UK.

出版信息

Pathogens. 2020 Jul 20;9(7):590. doi: 10.3390/pathogens9070590.

Abstract

Human cytomegalovirus (HCMV) establishes either a latent (non-productive) or lytic (productive) infection depending upon cell type, cytokine milieu and the differentiation status of the infected cell. Undifferentiated cells, such as precursor cells of the myeloid lineage, support a latent infection whereas terminally differentiated cells, such as monocytes or dendritic cells are an environment conducive to reactivation and support a lytic infection. The mechanisms which regulate HCMV in either a latent or lytic infection have been the focus of intense investigation with a view to developing novel treatments for HCMV-associated disease which can have a heavy clinical burden after reactivation or primary infection in, especially, the immune compromised. To this end, a number of studies have been carried out in an unbiased manner to address global changes occurring within the latently infected cell to address the molecular changes associated with HCMV latency. In this review, we will concentrate on the proteomic analyses which have been carried out in undifferentiated myeloid cells which either stably express specific viral latency associated genes in isolation or on cells which have been latently infected with virus.

摘要

人类巨细胞病毒(HCMV)根据细胞类型、细胞因子环境以及受感染细胞的分化状态,建立潜伏(非增殖性)或裂解(增殖性)感染。未分化细胞,如髓系谱系的前体细胞,支持潜伏感染,而终末分化细胞,如单核细胞或树突状细胞,则是有利于病毒重新激活并支持裂解感染的环境。调节HCMV潜伏或裂解感染的机制一直是深入研究的重点,目的是开发针对HCMV相关疾病的新疗法,尤其是在免疫功能低下患者中,病毒重新激活或初次感染后,HCMV相关疾病会带来沉重的临床负担。为此,已经开展了一些无偏向性的研究,以探讨潜伏感染细胞内发生的整体变化,从而了解与HCMV潜伏相关的分子变化。在这篇综述中,我们将集中讨论在未分化髓系细胞中进行的蛋白质组学分析,这些细胞要么单独稳定表达特定的病毒潜伏相关基因,要么被病毒潜伏感染。

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