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本文引用的文献

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Reduction of otherwise remarkably stable virus-specific cytotoxic T lymphocyte memory by heterologous viral infections.通过异源病毒感染减少原本非常稳定的病毒特异性细胞毒性T淋巴细胞记忆。
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Fas and FasL in the homeostatic regulation of immune responses.Fas和FasL在免疫反应的稳态调节中。
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The roles of perforin- and Fas-dependent cytotoxicity in protection against cytopathic and noncytopathic viruses.穿孔素依赖性和Fas依赖性细胞毒性在抵御细胞病变病毒和非细胞病变病毒中的作用。
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Mature T cells of autoimmune lpr/lpr mice have a defect in antigen-stimulated suicide.自身免疫性lpr/lpr小鼠的成熟T细胞在抗原刺激下的自杀过程中存在缺陷。
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Virus persistence in acutely infected immunocompetent mice by exhaustion of antiviral cytotoxic effector T cells.通过耗尽抗病毒细胞毒性效应T细胞,病毒在急性感染的免疫健全小鼠中持续存在。
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Programmed cell death of T lymphocytes during acute viral infection: a mechanism for virus-induced immune deficiency.急性病毒感染期间T淋巴细胞的程序性细胞死亡:病毒诱导免疫缺陷的一种机制。
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7
Autoimmune gld mutation uncouples suicide and cytokine/proliferation pathways in activated, mature T cells.自身免疫性gld突变使活化的成熟T细胞中的自杀途径与细胞因子/增殖途径解偶联。
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Rapid quantitation of apoptosis in pure and heterogeneous cell populations using flow cytometry.使用流式细胞术对纯细胞群体和异质细胞群体中的细胞凋亡进行快速定量分析。
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9
A specific intercellular pathway of apoptotic cell death is defective in the mature peripheral T cells of autoimmune lpr and gld mice.在自身免疫性lpr和gld小鼠的成熟外周T细胞中,凋亡性细胞死亡的一种特定细胞间途径存在缺陷。
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10
The Fas protein is expressed at high levels on CD4+CD8+ thymocytes and activated mature lymphocytes in normal mice but not in the lupus-prone strain, MRL lpr/lpr.在正常小鼠中,Fas蛋白在CD4+CD8+胸腺细胞和活化的成熟淋巴细胞上高水平表达,但在狼疮易感品系MRL lpr/lpr小鼠中则不表达。
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急性病毒感染后T淋巴细胞的下调不依赖于CD95(Fas)受体-配体相互作用。

T-lymphocyte downregulation after acute viral infection is not dependent on CD95 (Fas) receptor-ligand interactions.

作者信息

Lohman B L, Razvi E S, Welsh R M

机构信息

Department of Pathology, University of Massachusetts Medical Center, Worcester 01655, USA.

出版信息

J Virol. 1996 Nov;70(11):8199-203. doi: 10.1128/JVI.70.11.8199-8203.1996.

DOI:10.1128/JVI.70.11.8199-8203.1996
PMID:8892953
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC190902/
Abstract

Infection of mice with lymphocytic choriomeningitis virus (LCMV) causes a major expansion of CD8+ T cells followed by a period of immune downregulation that coincides with the induction of lymphocyte apoptosis in the mouse spleen. CD95 (Fas) and its ligand are important for regulating peripheral T-lymphocyte numbers and can mediate apoptosis of mature T lymphocytes. We infected CD95- and CD95L-deficient mice (lpr and gld, respectively) with LCMV to determine if the immune downregulation that occurred following resolution of the LCMV infection was due to a CD95-dependent apoptotic mechanism. Lymphocytes from LCMV-infected lpr and gld mice were capable of normal T-cell expansion and cytolytic function but were, in contrast to activated cells from normal virus-infected mice, relatively more resistant to T-cell receptor-induced apoptosis in vitro. However, in vivo there were significant numbers of apoptotic cells in the spleens of lpr and gld mice recovering from the infection, and the T-cell number and cytolytic activity decreased to normal postinfection levels. Thus, CD95 is not required for the immune downregulation of the CD8+-T-lymphocyte response following acute LCMV infection.

摘要

用淋巴细胞性脉络丛脑膜炎病毒(LCMV)感染小鼠会导致CD8 + T细胞大量扩增,随后进入免疫下调期,这与小鼠脾脏中淋巴细胞凋亡的诱导同时发生。CD95(Fas)及其配体对于调节外周T淋巴细胞数量很重要,并且可以介导成熟T淋巴细胞的凋亡。我们用LCMV感染了CD95和CD95L缺陷型小鼠(分别为lpr和gld),以确定LCMV感染消退后发生的免疫下调是否归因于CD95依赖性凋亡机制。来自LCMV感染的lpr和gld小鼠的淋巴细胞能够进行正常的T细胞扩增和细胞溶解功能,但与正常病毒感染小鼠的活化细胞相比,在体外对T细胞受体诱导的凋亡相对更具抗性。然而,在体内,从感染中恢复的lpr和gld小鼠脾脏中有大量凋亡细胞,并且T细胞数量和细胞溶解活性下降至感染后正常水平。因此,急性LCMV感染后CD8 + T淋巴细胞反应的免疫下调不需要CD95。