Somatic hypermutation generates a myriad of Ab mutants in Ag-specific B cells, from which high-affinity mutants are selected. Chickens, sheep, and rabbits use nontemplated point mutations and templated mutations via gene conversion to diversify their expressed Ig loci, whereas mice and humans rely solely on untemplated somatic point mutations. In this study, we demonstrate that, in addition to untemplated point mutations, templated mutagenesis readily occurs at the murine and human Ig loci. We provide two distinct lines of evidence that are not explained by the Neuberger model of somatic hypermutation: 1) across multiple data sets there is significant linkage disequilibrium between individual mutations, especially among close mutations, and 2) among those mutations, those <8 bp apart are significantly more likely to match microhomologous regions in the IgHV repertoire than predicted by the mutation profiles of somatic hypermutation. Together, this supports the role of templated mutagenesis during somatic diversification of Ag-activated B cells.
Clustered Mutations at the Murine and Human IgH Locus Exhibit Significant Linkage Consistent with Templated Mutagenesis.
小鼠和人类 IgH 基因座的聚集性突变表现出显著的连锁性,与模板诱变一致
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作者:Dale Gordon A, Wilkins Daniel J, Bohannon Caitlin D, Dilernia Dario, Hunter Eric, Bedford Trevor, Antia Rustom, Sanz Ignacio, Jacob Joshy
| 期刊: | Journal of Immunology | 影响因子: | 3.400 |
| 时间: | 2019 | 起止号: | 2019 Sep 1; 203(5):1252-1264 |
| doi: | 10.4049/jimmunol.1801615 | 种属: | Human |
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