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首页> 外文期刊>Genes and immunity. >Location and length distribution of somatic hypermutation-associated DNA insertions and deletions reveals regions of antibody structural plasticity
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Location and length distribution of somatic hypermutation-associated DNA insertions and deletions reveals regions of antibody structural plasticity

机译:体细胞高突变相关的DNA插入和缺失的位置和长度分布揭示了抗体结构可塑性的区域

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摘要

Following the initial diversity generated by V(D)J recombination, somatic hypermutation is the principal mechanism for producing further antibody repertoire diversity in antigen-experienced B cells. While somatic hypermutation typically results in single-nucleotide substitutions, the infrequent incorporation of genetic insertions and deletions has also been associated with the somatic hypermutation process. We used high-throughput antibody sequencing to determine the sequence of thousands of antibody genes containing somatic hypermutation-associated insertions and deletions (SHA indels), which revealed significant differences between the location of SHA indels and somatic mutations. Further, we identified a cluster of insertions and deletions in the antibody framework 3 region, which corresponds to the hypervariable region 4 (HV4) in T-cell receptors. We propose that this HV4-like region, identified by SHA indel analysis, represents a region of under-appreciated affinity maturation potential. Finally, through the analysis of both location and length distribution of SHA indels, we have determined regions of structural plasticity within the antibody protein.
机译:继通过V(D)J重组产生最初的多样性之后,体细胞超突变是在经历了抗原的B细胞中产生进一步的抗体库多样性的主要机制。虽然体细胞超突变通常导致单核苷酸取代,但是基因插入和缺失的不频繁掺入也与体细胞超突变过程有关。我们使用高通量抗体测序来确定数千个包含体细胞超突变相关插入和缺失(SHA indels)的抗体基因的序列,这揭示了SHA indels位置与体细胞突变之间的显着差异。此外,我们在抗体框架3区域中识别出一系列插入和缺失,该区域与T细胞受体中的高变区域4(HV4)相对应。我们提出,通过SHA indel分析鉴定的该类HV4区域代表了亲和力成熟潜力未得到充分认识的区域。最后,通过分析SHA插入缺失的位置和长度分布,我们确定了抗体蛋白内的结构可塑性区域。

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