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延长培养条件下小鼠T淋巴细胞产生白细胞介素-4的与年龄相关的下降。

Age-associated decline in IL-4 production by murine T lymphocytes in extended culture.

作者信息

Li S P, Miller R A

机构信息

Institute of Gerontology, University of Michigan, Ann Arbor.

出版信息

Cell Immunol. 1993 Oct 1;151(1):187-95. doi: 10.1006/cimm.1993.1230.

DOI:10.1006/cimm.1993.1230
PMID:8104710
Abstract

Aging leads to an increase in the proportion of cells that have the surface phenotype (CD45RBlo, CD44hi) characteristic of memory T lymphocytes and also to a decline in both the production of IL-2 and the response to this lymphokine. Several groups have reported an increase, with age, in the secretion of IL-4 in short-term T cell cultures and have suggested that this increase could reflect the age-dependent accumulation of memory T cells, which are thought to be principally responsible for IL-4 production in young mice. Because the response to IL-2 declines with age, we hypothesized that IL-4 production would also decline with age if tested under conditions that promoted IL-2-driven expansion and maturation of IL-4-secreting effectors. Using a culture system in which T cells are first activated by immobilized anti-CD3 antibody for 2 days, and then cultured with anti-CD3 plus IL-2 for an additional 9-11 days, we found a 3-fold decline with age in IL-4 production by murine splenic CD4 T cells. Under these conditions memory (CD45RBlo) CD4 T cells from young mice produced 22-fold more IL-4 than the reciprocal naive (CD44lo) subset. Production of IL-4 by old T cells was also largely attributable to memory T cells, but memory cells from these old donors generated 6-fold less IL-4 in extended cultures than memory cells from young donors. Cultured memory (but not naive) T cells increase in number over a 9-day interval, but the amount of expansion by young memory cells is 4-fold higher than that for old cells. We conclude that the production of IL-4 by memory T cells declines with age under conditions that promote IL-2-driven proliferation and differentiation.

摘要

衰老导致具有记忆性T淋巴细胞表面表型(CD45RBlo、CD44hi)特征的细胞比例增加,同时还导致白细胞介素-2(IL-2)的产生及对该淋巴因子的反应均下降。几个研究小组报告称,在短期T细胞培养中,IL-4的分泌会随着年龄的增长而增加,并认为这种增加可能反映了记忆性T细胞随年龄增长的积累,而记忆性T细胞被认为是幼鼠中IL-4产生的主要原因。由于对IL-2的反应会随着年龄的增长而下降,我们推测,如果在促进IL-2驱动的IL-4分泌效应细胞扩增和成熟的条件下进行检测,IL-4的产生也会随着年龄的增长而下降。使用一种培养系统,其中T细胞首先被固定化的抗CD3抗体激活2天,然后再与抗CD3加IL-2一起培养9 - 11天,我们发现小鼠脾脏CD4 T细胞产生的IL-4随着年龄增长下降了3倍。在这些条件下,来自幼鼠的记忆性(CD45RBlo)CD4 T细胞产生的IL-4比相应的初始(CD44lo)亚群多22倍。老年T细胞产生的IL-4在很大程度上也归因于记忆性T细胞,但这些老年供体的记忆细胞在延长培养中产生的IL-4比年轻供体的记忆细胞少6倍。培养的记忆性(而非初始)T细胞数量在9天的间隔内会增加,但年轻记忆细胞的扩增量比老年细胞高4倍。我们得出结论,在促进IL-2驱动的增殖和分化的条件下,记忆性T细胞产生的IL-4会随着年龄增长而下降。

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