免疫衰老
免疫学
医学
免疫系统
表型
衰老
人口
生物
肾脏疾病
细胞免疫
T细胞
疾病
遗传学
病理
内分泌学
基因
环境卫生
作者
Γεώργιος Λιούλιος,Asimina Fylaktou,Αikaterini Papagianni,Μaria Stangou
标识
DOI:10.1016/j.clim.2021.108685
摘要
Aging results in substantial changes in almost all cellular subpopulations within the immune system, including functional and phenotypic alterations. T lymphocytes, as the main representative population of cellular immunity, have been extensively studied in terms of modifications and adjustments during aging. Phenotypic alterations are attributed to three main mechanisms; a reduction of naive T cell population with a shift to more differentiated forms, a subsequent oligoclonal expansion of naive T cells characterized by repertoire restriction, and replicative insufficiency after repetitive activation. These changes and the subsequent phenotypic disorders are comprised in the term immunosenescence. Similar changes seem to occur in chronic kidney disease, with T cells of young patients resembling those of healthy older individuals. A broad range of surface markers can be utilized to identify immunosenescent T cells. In this review, we will discuss the most important senescence markers and their potential connection with impaired renal function.
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