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CD28表达的调节:激活和复制性衰老过程中的不同调控途径。

Modulation of CD28 expression: distinct regulatory pathways during activation and replicative senescence.

作者信息

Vallejo A N, Brandes J C, Weyand C M, Goronzy J J

机构信息

Division of Rheumatology, Department of Medicine, Mayo Clinic and Foundation, Rochester, MN 55905, USA.

出版信息

J Immunol. 1999 Jun 1;162(11):6572-9.

Abstract

The costimulatory molecule CD28 has a restricted tissue distribution and is expressed on T cells and some plasmacytoma cells. Although CD28 is constitutively expressed, its expression is transiently down-regulated following T cell activation and declines progressively with in vitro senescence. In vivo, CD8+ T cells and, less frequently, CD4+ T cells may completely lose CD28 surface expression during chronic infections and with aging. This correlates with changes of nuclear protein-binding activities to two motifs, site alpha and beta, within the CD28 minimal promoter. Both alpha- and beta-bound complexes are found only in lymphoid tissues, in CD28+ T cells, and in some transformed B cells. These complexes are coordinately expressed except during replicative senescence, which is characterized by the down-modulation of site beta- but not site alpha-binding activities. In contrast, T cell activation induces a parallel decline in both site alpha- and beta-binding activities. CD4+ and CD8+ T cells differ in their beta-binding profiles, which may explain the more pronounced down-regulation of CD28 in senescent CD8+ T cells. In vivo expanded CD4+CD28null and CD8+CD28null T cells uniformly lack alpha- and beta-bound complexes, resembling the pattern seen in chronically activated cells and not of senescent cells.

摘要

共刺激分子CD28具有有限的组织分布,表达于T细胞和一些浆细胞瘤细胞上。尽管CD28组成性表达,但其表达在T细胞活化后会短暂下调,并随着体外衰老而逐渐下降。在体内,CD8⁺ T细胞以及较少见的CD4⁺ T细胞在慢性感染和衰老过程中可能会完全丧失CD28表面表达。这与核蛋白与CD28最小启动子内两个基序(α位点和β位点)的结合活性变化相关。α结合复合物和β结合复合物仅在淋巴组织、CD28⁺ T细胞以及一些转化的B细胞中发现。这些复合物协同表达,除了在复制性衰老期间,复制性衰老的特征是β位点结合活性下调而α位点结合活性未下调。相反,T细胞活化会导致α位点和β位点结合活性同时下降。CD4⁺和CD8⁺ T细胞在其β结合谱上存在差异,这可能解释了衰老的CD8⁺ T细胞中CD28下调更为明显的现象。体内扩增的CD4⁺CD28⁰和CD8⁺CD28⁰ T细胞均缺乏α结合复合物和β结合复合物,类似于在长期活化细胞而非衰老细胞中所见的模式。

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