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DNA targets of AID evolutionary link between antibody somatic hypermutation and class switch recombination.

机译:抗体体细胞超突变与类别转换重组之间的AID进化联系的DNA靶点。

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摘要

As part of the adaptive immune response, B cells alter their functional immunoglobulin (Ig) receptor genes through somatic hypermutation (SHM) and/or class switch recombination (CSR) via processes that are initiated by activation induced cytidine deaminase (AID). These genetic modifications are targeted at specific sequences known as Variable (V) and Switch (S) regions. Here, we analyze and review the properties and function of AID target sequences across species and compare them with non-Ig sequences, including known translocation hotspots. We describe properties of the S sequences, and discuss species and isotypic differences among S regions. Common properties of SHM and CSR target sequences suggest that evolution of S regions might involve the duplication and selection of SHM hotspots.
机译:作为适应性免疫应答的一部分,B细胞通过激活诱导的胞苷脱氨酶(AID)引发的过程,通过体细胞超突变(SHM)和/或类别转换重组(CSR)来改变其功能性免疫球蛋白(Ig)受体基因。这些遗传修饰针对特定的序列,称为可变(V)和开关(S)区。在这里,我们分析和审查跨物种的AID目标序列的性质和功能,并将其与非Ig序列(包括已知的易位热点)进行比较。我们描述了S序列的属性,并讨论了S区域之间的物种和同型差异。 SHM和CSR目标序列的共同特性表明,S区的进化可能涉及SHM热点的复制和选择。

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