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Restoration of cytomegalovirus antigen presentation by gamma interferon combats viral escape.γ干扰素恢复巨细胞病毒抗原呈递可对抗病毒逃逸。
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Human cytomegalovirus-infected cells have unstable assembly of major histocompatibility complex class I complexes and are resistant to lysis by cytotoxic T lymphocytes.人巨细胞病毒感染的细胞具有不稳定的主要组织相容性复合体I类复合物组装,并且对细胞毒性T淋巴细胞的裂解具有抗性。
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Down-regulation of major histocompatibility complex class I synthesis by murine cytomegalovirus early gene expression.小鼠巨细胞病毒早期基因表达对主要组织相容性复合体I类合成的下调作用。
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Identification and expression of a murine cytomegalovirus early gene coding for an Fc receptor.编码Fc受体的小鼠巨细胞病毒早期基因的鉴定与表达
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Herpes simplex virus turns off the TAP to evade host immunity.单纯疱疹病毒关闭抗原加工相关转运体以逃避宿主免疫。
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Downregulation of peptide transporter genes in cell lines transformed with the highly oncogenic adenovirus 12.在被高度致癌的腺病毒12转化的细胞系中肽转运蛋白基因的下调。
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影响主要组织相容性复合体I类分子转运的小鼠巨细胞病毒基因组区域的鉴定。

Identification of the mouse cytomegalovirus genomic region affecting major histocompatibility complex class I molecule transport.

作者信息

Thäle R, Szepan U, Hengel H, Geginat G, Lucin P, Koszinowski U H

机构信息

Department of Virology, University of Heidelberg, Germany.

出版信息

J Virol. 1995 Oct;69(10):6098-105. doi: 10.1128/JVI.69.10.6098-6105.1995.

DOI:10.1128/JVI.69.10.6098-6105.1995
PMID:7666513
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC189506/
Abstract

Mouse cytomegalovirus (MCMV) functions expressed at the beginning of the early phase of the viral replication cycle interfere with the major histocompatibility complex (MHC) class I-restricted pathway of antigen presentation (M. J. Reddehase, M. R. Fibi, G. M. Keil, and U. H. Koszinowski, J. Virol. 60:1125-1129, 1986; M. Del Val, K. Münch, M. J. Reddehase, and U. H. Koszinowski, Cell 58:305-315, 1989). Nascent MHC class I heavy chains associate with beta 2-microglobulin and peptide, but the assembled trimolecular complex is retained in the endoplasmatic reticulum/cis-Golgi compartment (M. Del Val, H. Hengel, H. Häcker, U. Hartlaub, T. Ruppert, P. Lucin, and U. H. Koszinowski, J. Exp. Med. 176:729-738, 1992). To locate the responsible genomic region, the cytoplasmic retention of MHC class I molecules after injection of MCMV DNA was tested. The function was mapped to the HindIII E fragment. A recombinant MCMV deletion mutant delta MS94.5 lacking 15.8 kb in HindIII-E was constructed. Restoration of MHC class I molecule maturation and recognition of antigenic peptides by cytolytic T lymphocytes during the first hours of the early phase in mutant virus-infected cells proved the correct location to a 6.8-kb region in the HindIII E fragment. At later stages of the early phase, membrane-resident MHC class I molecules and cytolytic T lymphocyte recognition disappeared in delta MS94.5 mutant virus-infected cells. These results demonstrate that more than one early-gene function of MCMV affects the MHC class I pathway of antigen presentation. The redundant MHC class I-reactive functions target the transport of MHC class I molecules at different steps.

摘要

小鼠巨细胞病毒(MCMV)在病毒复制周期早期开始时表达的功能会干扰主要组织相容性复合体(MHC)I类限制的抗原呈递途径(M. J. 雷德哈斯、M. R. 菲比、G. M. 凯尔和U. H. 科斯齐诺夫斯基,《病毒学杂志》60:1125 - 1129,1986;M. 德尔瓦尔、K. 明希、M. J. 雷德哈斯和U. H. 科斯齐诺夫斯基,《细胞》58:305 - 315,1989)。新生的MHC I类重链与β2 - 微球蛋白和肽结合,但组装好的三分子复合物保留在内质网/顺式高尔基体区室中(M. 德尔瓦尔、H. 亨格尔、H. 哈克、U. 哈特劳布、T. 鲁珀特、P. 卢辛和U. H. 科斯齐诺夫斯基,《实验医学杂志》176:729 - 738,1992)。为了定位负责的基因组区域,检测了注射MCMV DNA后MHC I类分子的胞质滞留情况。该功能被定位到HindIII E片段。构建了一个在HindIII - E中缺失15.8 kb的重组MCMV缺失突变体δMS94.5。在突变病毒感染细胞的早期阶段的最初几个小时内,MHC I类分子成熟的恢复以及细胞毒性T淋巴细胞对抗原肽的识别证明了HindIII E片段中一个6.8 kb区域的定位正确。在早期阶段的后期,膜驻留的MHC I类分子和细胞毒性T淋巴细胞识别在δMS94.5突变病毒感染细胞中消失。这些结果表明,MCMV的不止一种早期基因功能影响MHC I类抗原呈递途径。冗余的MHC I类反应性功能在不同步骤靶向MHC I类分子的转运。