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T细胞衰老与人类长寿中的CD28表达

CD28 expression in T cell aging and human longevity.

作者信息

Boucher N, Dufeu-Duchesne T, Vicaut E, Farge D, Effros R B, Schächter F

机构信息

Centre d'Etude du Polymorphisme Humain, Paris, France.

出版信息

Exp Gerontol. 1998 May;33(3):267-82. doi: 10.1016/s0531-5565(97)00132-0.

Abstract

Functional decrements of the immune system have a major contribution to aging and age-related diseases. Here, we further characterize the decline in proportion of CD28-positive T cells previously identified in centenarians. Cohorts of 97 centenarians, 40 subjects aged 70-90 (ELD group), and 40 young adults (under age 40) were phenotyped for T cell surface expression of CD28, CD4, and CD8 antigens. The significant decline in T cells expressing CD28 (p < 10(-4) for comparisons between adults and either ELD or centenarians) affects preferentially the CD8+ subset of T cells. This decline accounts largely for the age-related diminution of T cell responsiveness to mitogenic signals. CD28 expression is modulated in T cell cultures in a growth-related fashion and this modulation is dampened in cultures from centenarians. We propose that the decrease in CD28 expression reflects a compensatory adaptation of the immune system during aging in the face of chronic stimulation.

摘要

免疫系统的功能衰退对衰老及与年龄相关的疾病有重大影响。在此,我们进一步描述了此前在百岁老人中发现的CD28阳性T细胞比例下降的情况。对97名百岁老人、40名70 - 90岁的受试者(老年组)以及40名年轻人(40岁以下)进行队列研究,分析其T细胞表面CD28、CD4和CD8抗原的表达情况。表达CD28的T细胞显著减少(与成年人和老年组或百岁老人组相比,p < 10(-4)),且优先影响T细胞的CD8 + 亚群。这种减少在很大程度上解释了与年龄相关的T细胞对有丝分裂信号反应性的降低。CD28表达在T细胞培养中以与生长相关的方式受到调节,而在百岁老人的培养物中这种调节受到抑制。我们提出,CD28表达的降低反映了衰老过程中免疫系统面对慢性刺激时的一种代偿性适应。

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