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在小鼠肺部潜伏性巨细胞病毒感染期间,肺部CD62L(lo)记忆效应细胞池中即时早期1(m123/pp89)肽特异性CD8 T细胞的富集。

Enrichment of immediate-early 1 (m123/pp89) peptide-specific CD8 T cells in a pulmonary CD62L(lo) memory-effector cell pool during latent murine cytomegalovirus infection of the lungs.

作者信息

Holtappels R, Pahl-Seibert M F, Thomas D, Reddehase M J

机构信息

Institute for Virology, Johannes Gutenberg University, 55101 Mainz, Germany.

出版信息

J Virol. 2000 Dec;74(24):11495-503. doi: 10.1128/jvi.74.24.11495-11503.2000.

Abstract

Interstitial cytomegalovirus (CMV) pneumonia is a clinically relevant complication in recipients of bone marrow transplantation (BMT). Recent data for a model of experimental syngeneic BMT and concomitant infection of BALB/c mice with murine CMV (mCMV) have documented the persistence of tissue-resident CD8 T cells after clearance of productive infection of the lungs (J. Podlech, R. Holtappels, M.-F. Pahl-Seibert, H.-P. Steffens, and M. J. Reddehase, J. Virol. 74:7496-7507, 2000). It was proposed that these cells represent antiviral "standby" memory cells whose functional role might be to help prevent reactivation of latent virus. The pool of pulmonary CD8 T cells was composed of two subsets defined by the T-cell activation marker L-selectin (CD62L): a CD62L(hi) subset of quiescent memory cells, and a CD62L(lo) subset of recently resensitized memory-effector cells. In this study, we have continued this line of investigation by quantitating CD8 T cells specific for the three currently published antigenic peptides of mCMV: peptide YPHFMPTNL processed from the immediate-early protein IE1 (pp89), and peptides YGPSLYRRF and AYAGLFTPL, derived from the early proteins m04 (gp34) and M84 (p65), respectively. IE1-specific CD8 T cells dominated in acute-phase pulmonary infiltrates and were selectively enriched in latently infected lungs. Notably, most IE1-specific CD8 T cells were found to belong to the CD62L(lo) subset representing memory-effector cells. This finding is in accordance with the interpretation that IE1-specific CD8 T cells are frequently resensitized during latent infection of the lungs and may thus be involved in the maintenance of mCMV latency.

摘要

间质性巨细胞病毒(CMV)肺炎是骨髓移植(BMT)受者临床上的一种相关并发症。最近关于同基因BMT实验模型以及BALB/c小鼠同时感染鼠巨细胞病毒(mCMV)的数据表明,肺部生产性感染清除后组织驻留CD8 T细胞持续存在(J. Podlech、R. Holtappels、M.-F. Pahl-Seibert、H.-P. Steffens和M. J. Reddehase,《病毒学杂志》74:7496 - 7507,2000年)。有人提出这些细胞代表抗病毒“备用”记忆细胞,其功能作用可能是帮助预防潜伏病毒的重新激活。肺部CD8 T细胞库由两个由T细胞活化标志物L - 选择素(CD62L)定义的亚群组成:静止记忆细胞的CD62L(hi)亚群和最近重新致敏的记忆效应细胞的CD62L(lo)亚群。在本研究中,我们通过定量针对目前已发表的mCMV三种抗原肽的CD8 T细胞继续了这一研究方向:从即刻早期蛋白IE1(pp89)加工而来的肽YPHFMPTNL,以及分别源自早期蛋白m04(gp34)和M84(p65)的肽YGPSLYRRF和AYAGLFTPL。IE1特异性CD8 T细胞在急性期肺部浸润中占主导地位,并在潜伏感染的肺部中选择性富集。值得注意的是,发现大多数IE1特异性CD8 T细胞属于代表记忆效应细胞的CD62L(lo)亚群。这一发现符合以下解释:IE1特异性CD8 T细胞在肺部潜伏感染期间经常重新致敏,因此可能参与mCMV潜伏状态的维持。

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