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本文引用的文献

1
Characterization of a novel Golgi apparatus-localized latency determinant encoded by human cytomegalovirus.人巨细胞病毒编码的一种新型高尔基体定位潜伏决定因子的特性分析。
J Virol. 2009 Jun;83(11):5615-29. doi: 10.1128/JVI.01989-08. Epub 2009 Mar 18.
2
Immunobiology of human cytomegalovirus: from bench to bedside.人类巨细胞病毒的免疫生物学:从 bench 到 bedside。 (注:bench 与 bedside 在这里可能是一种形象说法,bench 可理解为基础研究阶段,bedside 可理解为临床应用阶段,直译为“从实验台到病床边”,意译为“从基础研究到临床应用” ) 准确完整的译文:人类巨细胞病毒的免疫生物学:从基础研究到临床应用
Clin Microbiol Rev. 2009 Jan;22(1):76-98, Table of Contents. doi: 10.1128/CMR.00034-08.
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Dynamics of T cell memory in human cytomegalovirus infection.人类巨细胞病毒感染中T细胞记忆的动态变化
Med Microbiol Immunol. 2008 Jun;197(2):83-96. doi: 10.1007/s00430-008-0082-5. Epub 2008 Feb 27.
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Human cytomegalovirus: Latency and reactivation in the myeloid lineage.人巨细胞病毒:髓系细胞中的潜伏与激活
J Clin Virol. 2008 Mar;41(3):180-5. doi: 10.1016/j.jcv.2007.11.014.
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Expression of a human cytomegalovirus latency-associated homolog of interleukin-10 during the productive phase of infection.人巨细胞病毒白细胞介素-10潜伏相关同源物在感染增殖期的表达。
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Massive load of functional effector CD4+ and CD8+ T cells against cytomegalovirus in very old subjects.极老年受试者体内存在大量针对巨细胞病毒的功能性效应CD4+和CD8+ T细胞。
J Immunol. 2007 Sep 15;179(6):4283-91. doi: 10.4049/jimmunol.179.6.4283.
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Human cytomegalovirus sequences expressed in latently infected individuals promote a latent infection in vitro.在潜伏感染个体中表达的人巨细胞病毒序列可在体外促进潜伏感染。
Blood. 2007 Aug 1;110(3):937-45. doi: 10.1182/blood-2007-01-070078. Epub 2007 Apr 17.
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Cellular responses to viral infection in humans: lessons from Epstein-Barr virus.人类细胞对病毒感染的反应:来自爱泼斯坦-巴尔病毒的启示。
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9
Influence of translation efficiency of homologous viral proteins on the endogenous presentation of CD8+ T cell epitopes.同源病毒蛋白翻译效率对CD8+ T细胞表位内源性呈递的影响。
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10
Viral gene expression during the establishment of human cytomegalovirus latent infection in myeloid progenitor cells.人巨细胞病毒在髓系祖细胞中建立潜伏感染期间的病毒基因表达
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CD8+ T 细胞对人巨细胞病毒潜伏相关决定簇 pUL138 的识别。

CD8+ T-cell recognition of human cytomegalovirus latency-associated determinant pUL138.

机构信息

School of Medicine, University of Queensland, Brisbane, Australia.

Australian Centre for Vaccine Development and Tumour Immunology Laboratory, Division of Immunology, Queensland Institute of Medical Research, Brisbane, Australia.

出版信息

J Gen Virol. 2010 Aug;91(Pt 8):2040-2048. doi: 10.1099/vir.0.020982-0. Epub 2010 Apr 7.

DOI:10.1099/vir.0.020982-0
PMID:20375220
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4091183/
Abstract

Recent studies have shown that long-term persistence of human cytomegalovirus (HCMV) in mononuclear cells of myeloid lineage is dependent on the UL138 open reading frame, which promotes latent infection. Although T-cell recognition of protein antigens from all stages of lytic HCMV infection is well established, it is not clear whether proteins expressed during latent HCMV infection can also be recognized. This study conducted an analysis of T-cell response towards proteins associated with HCMV latency. Ex vivo analysis of T cells from healthy virus carriers revealed a dominant CD8(+) T-cell response to the latency-associated pUL138 protein, which recognized a non-canonical 13 aa epitope in association with HLA-B*3501. These pUL138-specific T cells displayed a range of memory phenotypes that were in general less differentiated than that previously described in T cells specific for HCMV lytic antigens. Antigen-presentation assays revealed that endogenous pUL138 could be presented efficiently by HCMV-infected cells. However, T-cell recognition of pUL138 was dependent on newly synthesized protein, with little presentation from stable, long-lived protein. These data demonstrate that T cells targeting latency-associated protein products exist, although HCMV may limit the presentation of latent proteins, thereby restricting T-cell recognition of latently infected cells.

摘要

最近的研究表明,人类巨细胞病毒(HCMV)在髓样谱系单核细胞中的长期持续存在依赖于 UL138 开放阅读框,该阅读框促进潜伏感染。虽然 T 细胞对所有裂解 HCMV 感染阶段的蛋白抗原的识别已得到充分证实,但尚不清楚潜伏 HCMV 感染期间表达的蛋白是否也能被识别。本研究对与 HCMV 潜伏相关的蛋白的 T 细胞反应进行了分析。对健康病毒携带者的 T 细胞进行体外分析显示,针对潜伏相关 pUL138 蛋白的 CD8(+) T 细胞反应占主导地位,该蛋白与 HLA-B*3501 结合识别一个非典型的 13 个氨基酸表位。这些 pUL138 特异性 T 细胞表现出一系列记忆表型,通常比以前描述的针对 HCMV 裂解抗原的 T 细胞分化程度低。抗原呈递实验表明,内源性 pUL138 可以被 HCMV 感染的细胞有效呈递。然而,pUL138 的 T 细胞识别依赖于新合成的蛋白,而稳定的、寿命长的蛋白几乎没有呈递。这些数据表明,存在针对潜伏相关蛋白产物的 T 细胞,尽管 HCMV 可能限制潜伏蛋白的呈递,从而限制了 T 细胞对潜伏感染细胞的识别。