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The analysis of clonal expansions in normal and autoimmune B cell repertoires

机译:正常和自身免疫性B细胞库中克隆扩增的分析

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摘要

Clones are the fundamental building blocks of immune repertoires. The number of different clones relates to the diversity of the repertoire, whereas their size and sequence diversity are linked to selective pressures. Selective pressures act both between clones and within different sequence variants of a clone. Understanding how clonal selection shapes the immune repertoire is one of the most basic questions in all of immunology. But how are individual clones defined? Here we discuss different approaches for defining clones, starting with how antibodies are diversified during different stages of B cell development. Next, we discuss how clones are defined using different experimental methods. We focus on high-throughput sequencing datasets, and the computational challenges and opportunities that these data have for mining the antibody repertoire landscape. We discuss methods that visualize sequence variants within the same clone and allow us to consider collections of shared mutations to determine which sequences share a common ancestry. Finally, we comment on features of frequently encountered expanded B cell clones that may be of particular interest in the setting of autoimmunity and other chronic conditions.
机译:克隆是免疫库的基本组成部分。不同克隆的数量与库的多样性有关,而其大小和序列的多样性则与选择压力有关。选择压力在克隆之间以及克隆的不同序列变体中均起作用。理解克隆选择如何影响免疫系统是所有免疫学中最基本的问题之一。但是如何定义单个克隆?在这里,我们讨论定义克隆的不同方法,首先从在B细胞发育的不同阶段如何多样化抗体开始。接下来,我们讨论如何使用不同的实验方法定义克隆。我们专注于高通量测序数据集,以及这些数据在挖掘抗体库景观方面的计算挑战和机遇。我们讨论了可视化同一克隆中序列变异的方法,并允许我们考虑共享突变的集合,以确定哪些序列具有共同的血统。最后,我们评论了经常遇到的扩展B细胞克隆的特征,这些特征在自身免疫性疾病和其他慢性疾病的治疗中可能特别有意义。

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