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首页> 外文期刊>Arthritis Research >Ageing, autoimmunity and arthritis: Senescence of the B cell compartment – implications for humoral immunity
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Ageing, autoimmunity and arthritis: Senescence of the B cell compartment – implications for humoral immunity

机译:衰老,自身免疫和关节炎:B细胞区室衰老–对体液免疫的影响

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Immunosenescence is associated with a decline in both T and B lymphocyte function. Although aged individuals have normal numbers of B cells in the periphery and are capable of mounting robust humoral responses, the antibodies produced are generally of lower affinity and are less protective than those produced by young animals. Here we review multiple studies that address the mechanisms that contribute to this decline. Taken together, these studies suggest that age-associated loss of the ability to generate protective humoral immunity results in part from reduced B lymphopoiesis. As the output of new, na?ve B cells declines, homeostatic pressures presumably force the filling of the peripheral B cell pool by long-lived antigen-experienced cells. Because the antibody repertoire of these cells is restricted by previous antigenic experience, they make poor quality responses to new immunologic insults.
机译:免疫衰老与T和B淋巴细胞功能的下降有关。尽管老年个体的外周血B细胞数量正常,并且能够引起强烈的体液反应,但是产生的抗体通常比幼小动物产生的亲和力低且保护性较低。在这里,我们回顾了针对导致这种下降的机制的多项研究。综上所述,这些研究表明,与年龄相关的产生保护性体液免疫能力的丧失部分归因于B淋巴细胞减少。随着新的幼稚B细胞的产量下降,稳态压力可能迫使长寿命的抗原经历细胞充盈外周B细胞。由于这些细胞的抗体库受以前的抗原经验的限制,因此它们对新的免疫学反应的质量反应较差。

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