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衰老与T细胞多样性

Aging and T-cell diversity.

作者信息

Goronzy Jörg J, Lee Won-Woo, Weyand Cornelia M

机构信息

Lowance Center for Human Immunology, Emory University School of Medicine, 101 Woodruff Circle #1003, Atlanta, GA 30322, USA.

出版信息

Exp Gerontol. 2007 May;42(5):400-6. doi: 10.1016/j.exger.2006.11.016. Epub 2007 Jan 10.

Abstract

Naïve and memory CD4 and CD8 T cells constitute a highly dynamic system with constant homeostatic and antigen-driven proliferation, influx, and loss of T cells. Thymic activity dwindles with age and essentially ceases in the later decades of life, severely constraining the generation of new T cells. Homeostatic control mechanisms are very effective at maintaining a large and diverse subset of naïve CD4 T cells through the 7th decade of life, but eventually and abruptly fail at about the age of 75 years. In contrast, the CD8 T cell compartment is more unstable, with progressive diminution of naïve T cells and increasing loss of diversity during mid adulthood. Vaccination strategies need to aim at developing a broad repertoire of memory T cells before the critical time period when the naïve CD4 T-cell repertoire collapses. Research efforts need to aim at understanding T-cell homeostatic control mechanisms to ultimately expand the time period of repertoire stability.

摘要

初始和记忆性CD4和CD8 T细胞构成了一个高度动态的系统,T细胞不断进行稳态和抗原驱动的增殖、流入及损耗。胸腺活性随年龄增长而下降,在生命的后几十年基本停止,严重限制了新T细胞的产生。稳态控制机制在维持大量多样的初始CD4 T细胞亚群方面非常有效,可贯穿生命的第七个十年,但最终在约75岁时突然失效。相比之下,CD8 T细胞区室更不稳定,在成年中期,初始T细胞逐渐减少,多样性丧失增加。疫苗接种策略需要旨在在初始CD4 T细胞库崩溃的关键时期之前,培养广泛的记忆T细胞库。研究工作需要旨在了解T细胞稳态控制机制,以最终延长库稳定性的时间段。

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