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Reconstructing a B-cell clonal lineage. I. Statistical inference of unobserved ancestors

机译:重建B细胞克隆谱系。一未观察到的祖先的统计推断

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摘要

One of the key phenomena in the adaptive immune response to infection and immunization is affinity maturation, during which antibody genes are mutated and selected, typically resulting in a substantial increase in binding affinity to the eliciting antigen. Advances in technology on several fronts have made it possible to clone large numbers of heavy-chain light-chain pairs from individual B cells and thereby identify whole sets of clonally related antibodies. These collections could provide the information necessary to reconstruct their own history - the sequence of changes introduced into the lineage during the development of the clone - and to study affinity maturation in detail. But the success of such a program depends entirely on accurately inferring the founding ancestor and the other unobserved intermediates. Given a set of clonally related immunoglobulin V-region genes, the method described here allows one to compute the posterior distribution over their possible ancestors, thereby giving a thorough accounting of the uncertainty inherent in the reconstruction.I demonstrate the application of this method on heavy-chain and light-chain clones, assess the reliability of the inference, and discuss the sources of uncertainty.
机译:对感染和免疫的适应性免疫反应中的关键现象之一是亲和力成熟,在此期间突变和选择抗体基因,通常会导致与引发抗原的结合亲和力大大提高。在几个方面的技术进步使得有可能从单个B细胞克隆大量重链轻链对,从而鉴定出完整的克隆相关抗体。这些集合可以提供重建其自身历史(在克隆形成过程中引入谱系的变化序列)以及详细研究亲和力成熟所必需的信息。但是,这样一个程序的成功完全取决于准确地推论创始祖先和其他未被观察到的中间体。给定一组克隆相关的免疫球蛋白V区基因,此处描述的方法允许一个人计算其可能祖先的后验分布,从而全面解释重建中固有的不确定性。链和轻链克隆,评估推断的可靠性,并讨论不确定性的来源。

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