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CD4 T cell defects in the aged: Causes, consequences and strategies to circumvent

机译:老年人CD4 T细胞缺陷:成因,后果和应对策略

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Aging leads to reduced immunity, especially adaptive responses. A key deficiency is the poor ability to mount robust antibody response. Although intrinsic alterations in B cells with age are in part responsible, impaired CD4 T cell help makes a major contribution to the poor antibody response. Other CD4 effector responses and memory generation are also impaired. We find delayed and reduced development of CD4 T follicular help (Tfh) cells in aged mice in response to influenza infection with reduction of long-lived plasma cells. When we examine CD4 subsets we also find a shift towards Thl and cytotoxic CD4 (ThCTL) responses. We summarize strategies to circumvent the CD4 T cell defect in aged, including adjuvants and proinflammatory cytokines. We find that we can strongly enhance responses of aged naive CD4 T cells by using Toll-like receptor (TLR) activated dendritic cells (DC) as APC in vivo and that this leads to improved germinal center B cells and IgG antibody responses. The enhanced response of aged naive CD4 T cells is dependent on IL-6 produced by the DC.
机译:衰老导致免疫力下降,尤其是适应性反应。一个关键的缺陷是,难以进行稳定的抗体反应。尽管随着年龄的增长,B细胞的内在变化是部分原因,但受损的CD4 T细胞帮助对不良抗体反应做出了重要贡献。其他CD4效应子的反应和记忆的产生也受到损害。我们发现延缓和减少CD4 T卵泡帮助(Tfh)细胞的衰老小鼠响应流感病毒感染减少了长寿浆细胞的发育。当我们检查CD4子集时,我们还发现向Th1和细胞毒性CD4(ThCTL)反应的转变。我们总结了规避老年人CD4 T细胞缺陷的策略,包括佐剂和促炎细胞因子。我们发现我们可以通过在体内使用Toll样受体(TLR)激活的树突状细胞(DC)作为APC来强烈增强衰老的原始CD4 T细胞的反应,并且这会导致生发中心B细胞和IgG抗体反应得到改善。衰老的幼稚CD4 T细胞的增强反应取决于DC产生的IL-6。

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