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由于CD4+和CD8+亚群中不同的克隆扩增导致人类αβ T细胞库的年龄相关改变。

Age-related modifications of the human alphabeta T cell repertoire due to different clonal expansions in the CD4+ and CD8+ subsets.

作者信息

Wack A, Cossarizza A, Heltai S, Barbieri D, D'Addato S, Fransceschi C, Dellabona P, Casorati G

机构信息

Unità d'Immunochimica, DIBIT, Istituto Scientifico H. San Raffaele, Milano, Italy.

出版信息

Int Immunol. 1998 Sep;10(9):1281-8. doi: 10.1093/intimm/10.9.1281.

DOI:10.1093/intimm/10.9.1281
PMID:9786427
Abstract

We have studied the effects of a life-long antigen stimulation on the clonal heterogeneity of human peripheral T cell subsets, as defined by their CD45 isoform expression. CD4+ or CD8+ T cells were obtained from healthy donors ranging in age from 20 to 100 years, and sorted into CD45RA+ and CD45RO+ populations. A modified PCR-heteroduplex analysis was then used to directly compare the TCR Vbeta clonal make up of either compartment pair. We find that the CD4+ T cell repertoire remains largely polyclonal throughout life, since CD4+ expanded clones are rare and accumulate predominantly in the CD45RO+ compartment of exceptionally old donors (100 years old). In contrast, the CD8+ T cell subset contains expanded clones which are already detectable in young adults and become very frequent in 70- to 75-year-old donors in both CD45RA+ and CD45RO+ compartments analyzed. Interestingly, some expanded clones are detectable in the CD45RA+ or in both CD45RA+ and CD45RO+ compartments of either CD4+ or CD8+ T cells. These results indicate that the age-dependent accumulation of expanded clones starts earlier and is more pronounced in the CD8+ than in the CD4+ T cell subset, reinforcing the concept that clonal expansion in the two subsets is controlled by substantially different mechanisms. Furthermore, whereas the finding of expanded CD45RO+ T cell clones is explained by antigen-driven proliferation, the detection of expanded clones in the CD45RA+ or in both CD45RA+ and CD45RO+ compartments would support the hypothesis of reversion from the CD45RO+ to the CD45RA+ phenotype after antigen encounter.

摘要

我们研究了终生抗原刺激对人外周血T细胞亚群克隆异质性的影响,这些亚群通过其CD45异构体表达来定义。从年龄在20至100岁的健康供体中获取CD4+或CD8+ T细胞,并将其分选成CD45RA+和CD45RO+群体。然后使用改良的PCR-异源双链分析直接比较任一亚群对的TCR Vβ克隆组成。我们发现,CD4+ T细胞库在一生中基本保持多克隆状态,因为CD4+扩增克隆很少见,且主要在特别年老的供体(100岁)的CD45RO+亚群中积累。相比之下,CD8+ T细胞亚群包含扩增克隆,这些克隆在年轻成年人中已可检测到,并且在分析的70至75岁供体的CD45RA+和CD45RO+亚群中变得非常常见。有趣的是,在CD4+或CD8+ T细胞的CD45RA+或CD45RA+和CD45RO+两个亚群中都可检测到一些扩增克隆。这些结果表明,扩增克隆的年龄依赖性积累在CD8+ T细胞亚群中比在CD4+ T细胞亚群中开始得更早且更明显,这强化了两个亚群中的克隆扩增由截然不同的机制控制的概念。此外,虽然CD45RO+ T细胞克隆扩增的发现可通过抗原驱动的增殖来解释,但在CD45RA+或CD45RA+和CD45RO+两个亚群中检测到扩增克隆将支持抗原接触后从CD45RO+表型逆转为CD45RA+表型的假说。

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