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Ageing of the B-cell repertoire

机译:B细胞库的老化

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Older people are more susceptible to infection, less responsive to vaccination and have a more inflammatory immune environment. Using spectratype analysis, we have previously shown that the B-cell repertoire of older people shows evidence of inappropriate clonal expansions in the absence of challenge, and that this loss of B-cell diversity correlates with poor health. Studies on response to vaccination, using both spectratyping and high-throughput sequencing of the repertoire, indicate that older responses to challenge are lacking in magnitude and/or delayed significantly. Also that some of the biologically significant differences may be in different classes of antibody. We have also previously shown that normal young B-cell repertoires can vary between different phenotypic subsets of B cells. In this paper, we present an analysis of immunoglobulin repertoire in different subclasses of antibody in five different populations of B cell, and show how the repertoire in these different groups changes with age. Although some age-related repertoire differences occur in naive cells, before exogenous antigen exposure, we see indications that there is a general dysregulation of the selective forces that shape memory B-cell populations in older people.
机译:老年人更容易受到感染,对疫苗的反应较弱,并且具有更炎性的免疫环境。使用光谱类型分析,我们以前已经证明,老年人的B细胞谱系在缺乏挑战的情况下显示了不适当的克隆扩增的证据,并且这种B细胞多样性的丧失与健康状况不佳相关。使用谱型和高通量测序对疫苗接种的反应进行的研究表明,对激发的较早反应缺乏强度和/或显着延迟。同样,某些生物学上的显着差异可能在抗体的不同类别中。先前我们还表明,正常的年轻B细胞库可以在B细胞的不同表型子集之间变化。在本文中,我们对五个不同的B细胞种群中不同抗体亚类的免疫球蛋白库进行了分析,并显示了这些不同组中库库如何随年龄变化。尽管幼稚细胞中存在一些与年龄相关的库差异,但在外源性抗原暴露之前,我们发现有迹象表明,塑造老年人记忆B细胞群体的选择性力普遍存在调节异常。

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