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Strong intrinsic biases towards mutation and conservation of bases in human IgVH genes during somatic hypermutation prevent statistical analysis of antigen selection.

机译:在体细胞高变过程中对人IgVH基因碱基的突变和保守性的强烈内在偏见阻止了抗原选择的统计分析。

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摘要

Immunoglobulin V region genes acquire point mutations during affinity maturation of the T-cell-dependent B-cell response. It has been proposed that both selection by antigen and characteristics of the DNA sequence are involved in determining the distribution of mutations along the genes. There is a tendency for replacement mutations to occur in the complementarity-determining regions and for silent mutations to accumulate in the framework regions of used genes. By analysing a group of highly mutated human IgVH4-34 (VH4. 21) and family 5 genes derived from human gut-associated lymphoid tissues, which were out-of-frame between VH and JH (and therefore not used) we have investigated the distribution of mutations acquired in the absence of selection. We observed that these genes may show the statistical hallmarks of selected genes, suggesting that intrinsic biases alone may be enough to give the appearance of selection. These data suggest that analysis of the distribution of mutations in IgVH genes cannot be used reliably to state whether antigenic selection of the B-cell carrying the genes occurred. In-frame genes had more silent mutations than the out-of-frame genes and lacked stop codons. These characteristics were considered to be indicative of selection in the in-frame genes derived from human gut-associated lymphoid tissue.
机译:免疫球蛋白V区基因在依赖T细胞的B细胞反应的亲和力成熟过程中获得点突变。已经提出,通过抗原的选择和DNA序列的特征都参与确定沿基因的突变的分布。有一种趋势是在决定互补性的区域发生替换突变,而沉默的突变则在使用的基因的构架区域中积累。通过分析一组高度突变的人IgVH4-34(VH4.21)和源自人肠相关淋巴组织的家族5基因,它们在VH和JH之间是不合框架的(因此未使用),我们研究了在没有选择的情况下获得的突变的分布。我们观察到这些基因可能显示所选基因的统计特征,表明仅固有的偏倚可能足以给出选择的外观。这些数据表明,不能可靠地使用IgVH基因突变分布的分析来说明是否发生了携带该基因的B细胞的抗原选择。框内基因比框外基因具有更多的沉默突变,并且缺少终止密码子。这些特征被认为指示在源自人肠相关淋巴组织的框内基因中的选择。

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