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预防CD2-fas转基因小鼠中与年龄相关的T细胞凋亡缺陷。

Prevention of age-related T cell apoptosis defect in CD2-fas-transgenic mice.

作者信息

Zhou T, Edwards C K, Mountz J D

机构信息

Veterans Administration Medical Center, Birmingham, Alabama, USA.

出版信息

J Exp Med. 1995 Jul 1;182(1):129-37. doi: 10.1084/jem.182.1.129.

DOI:10.1084/jem.182.1.129
PMID:7540646
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2192099/
Abstract

T cell dysfunction and thymic involution are major immunologic abnormalities associated with aging. Fas (CD95) is a bifunctional molecule that is critical for apoptosis and stimulation during T cell development, but the role of Fas during aging has not been determined. Fas expression and function on T cells from old (22-26-mo-old) mice was compared with young (2-mo-old) mice and old CD2-fas-transgenic mice. Fas expression and ligand-induced apoptosis were decreased on T cells from old mice compared with young mice. This correlated with an age-related increase in CD44+Fas- T cells. There was a marked decrease in the proliferation of T cells from old mice after anti-CD3 stimulation compared with young mice. Anti-CD3-stimulated T cells from young mice exhibited increased production of interleukin (IL)-2 and decreased production of interferon-gamma and IL-10 compared with old mice. There was an age-related decrease in the total thymocyte count from 127 +/- 10 cells in young mice compared with 26 +/- 8 x 10(6) in old mice. In 26-mo-old CD2-fas-transgenic mice, Fas and CD44 expression, Fas-induced apoptosis, T cell proliferation, and cytokine production were comparable to that of the young mice. These results suggest that T cell senescence with age is associated with defective apoptosis, and that the CD2-fas transgene allows maintenance of Fas apoptosis function and T cell function in aged mice comparable to that of young mice.

摘要

T细胞功能障碍和胸腺退化是与衰老相关的主要免疫异常。Fas(CD95)是一种双功能分子,对T细胞发育过程中的细胞凋亡和刺激至关重要,但Fas在衰老过程中的作用尚未确定。将老年(22 - 26月龄)小鼠T细胞上的Fas表达和功能与年轻(2月龄)小鼠及老年CD2 - Fas转基因小鼠进行比较。与年轻小鼠相比,老年小鼠T细胞上的Fas表达和配体诱导的细胞凋亡减少。这与CD44 + Fas - T细胞随年龄增长而增加相关。与年轻小鼠相比,抗CD3刺激后老年小鼠T细胞的增殖明显减少。与老年小鼠相比,年轻小鼠抗CD3刺激的T细胞表现出白细胞介素(IL)-2产生增加,干扰素 - γ和IL - 10产生减少。与年轻小鼠胸腺细胞总数(127±10个细胞)相比,老年小鼠胸腺细胞总数(26±8×10⁶个细胞)出现与年龄相关的减少。在26月龄的CD2 - Fas转基因小鼠中,Fas和CD44表达、Fas诱导的细胞凋亡、T细胞增殖和细胞因子产生与年轻小鼠相当。这些结果表明,随着年龄增长T细胞衰老与细胞凋亡缺陷有关,并且CD2 - Fas转基因可使老年小鼠维持与年轻小鼠相当的Fas凋亡功能和T细胞功能。

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