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老年人自然杀伤细胞的表型标志物及白细胞介素2反应

NK phenotypic markers and IL2 response in NK cells from elderly people.

作者信息

Borrego F, Alonso M C, Galiani M D, Carracedo J, Ramirez R, Ostos B, Peña J, Solana R

机构信息

Department of Immunology, Hospital Universitario Reina Sofia, Cordoba, Spain.

出版信息

Exp Gerontol. 1999 Apr;34(2):253-65. doi: 10.1016/s0531-5565(98)00076-x.

Abstract

Immunosenescence is a process that primarily affects the T cell compartment of the immune system, although age-associated immunological alterations have also been demonstrated in the NK cell phenotype and function. A significant expansion in the number of NK cells is found in aging. The NK cytotoxic capacity of total peripheral blood lymphocytes is also well preserved, not only in healthy elderly people but also in centenarians. However, NK cell killing of K562 is impaired when considered in a per-cell basis, and this defect is associated with defective signal transduction after activation more than a diminished conjugate formation or killing capacity. We have studied the phenotype of NK cells in elderly donors fulfilling the Senieur criteria. We have also studied the capacity of these cells to be activated by IL2 when different NK cell functions, other than cytotoxicity, are considered. Our results confirm the increased percentage of NK cells in the elderly due to the expansion of the CD56dim subset that also show an altered pattern of activation markers, whereas no differences were found in the CD56bright subset. The response of NK cells to IL2 was found to be impaired when proliferation, expression of CD69, and Ca2+ mobilization were considered, whereas TNF-alpha production was not significantly affected. These results suggest that human NK cells do not escape the aging process, although senescence have a differential effect on distinct NK cell biological functions, ranging from severe to negligible impairment, depending on the parameters considered.

摘要

免疫衰老主要影响免疫系统的T细胞区室,尽管在自然杀伤(NK)细胞表型和功能方面也已证实存在与年龄相关的免疫改变。在衰老过程中发现NK细胞数量显著增加。不仅在健康老年人中,而且在百岁老人中,外周血淋巴细胞的NK细胞毒性能力也得到了很好的保留。然而,以单个细胞为基础考虑时,NK细胞对K562的杀伤能力受损,这种缺陷与激活后信号转导缺陷有关,而不是共轭形成减少或杀伤能力下降。我们研究了符合老年标准的老年供体中NK细胞的表型。当考虑除细胞毒性之外的不同NK细胞功能时,我们还研究了这些细胞被白细胞介素-2(IL-2)激活的能力。我们的结果证实,由于CD56dim亚群的扩增,老年人中NK细胞的百分比增加,这些亚群还表现出激活标志物模式的改变,而在CD56bright亚群中未发现差异。当考虑增殖、CD69表达和钙离子动员时,发现NK细胞对IL-2的反应受损,而肿瘤坏死因子-α(TNF-α)的产生没有受到显著影响。这些结果表明,人类NK细胞无法逃避衰老过程,尽管衰老对不同的NK细胞生物学功能有不同的影响,根据所考虑的参数,从严重损害到可忽略不计的损害不等。

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