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多种鲨鱼免疫球蛋白重链基因可自主发生重排和超突变。

The multiple shark Ig H chain genes rearrange and hypermutate autonomously.

机构信息

Department of Physiology and Pharmacology, State University of New York Health Science Center at Brooklyn, Brooklyn, NY 11203, USA.

出版信息

J Immunol. 2011 Sep 1;187(5):2492-501. doi: 10.4049/jimmunol.1101671. Epub 2011 Jul 29.

Abstract

Sharks and skates are representatives of the earliest vertebrates with an immune system based on V(D)J rearrangement. They possess a unique Ig gene organization consisting of 15 to >50 individual IgM loci, each with one VH, two DH, one JH, and one set of constant region exons. The present study attempts to understand how multiple Ig genes are regulated with respect to rearrangement initiation and to targeting during somatic hypermutation. The linkage of three single-copy IgH genes was determined, and single-cell genomic PCR studies in a neonatal animal were used to examine any relationship between relative gene position and likelihood of rearrangement. Our results show that one to three IgH genes are activated independently of linkage or allelic position and the data best fit with a probability model based on the hypothesis that V(D)J rearrangement occurs as a sequence of trials within the B cell. In the neonatal cell set, two closely related IgH, G2A, and G2B, rearranged at similar frequencies, and their membrane forms were expressed at similar levels, like in other young animals. However, older animals displayed a bias in favor of the G2A isotype, which suggests that although rearrangement at G2A and G2B was randomly initiated during primary repertoire generation, the two very similar IgM sequences appear to be differentially expressed with age and exposure to Ag. We performed genomic single-cell PCR on B cells from an immunized individual to study activation-induced cytidine deaminase targeting and found that hypermutation, like V(D)J rearrangement, occurred independently among the many shark IgH.

摘要

鲨鱼和鳐鱼是最早的脊椎动物代表,其免疫系统基于 V(D)J 重排。它们具有独特的 Ig 基因组织,由 15 到 >50 个单独的 IgM 基因座组成,每个基因座都有一个 VH、两个 DH、一个 JH 和一组恒定区外显子。本研究试图了解在体细胞超突变过程中,多个 Ig 基因是如何被调控的,以启动重排和靶向。确定了三个单拷贝 IgH 基因的连锁,并在新生动物中单细胞基因组 PCR 研究用于检查相对基因位置和重排可能性之间的任何关系。我们的结果表明,一个到三个 IgH 基因独立于连锁或等位基因位置被激活,并且数据最符合基于 V(D)J 重排作为 B 细胞内一系列试验的假设的概率模型。在新生细胞集中,两个密切相关的 IgH、G2A 和 G2B 以相似的频率重排,并且它们的膜形式以相似的水平表达,就像在其他年幼的动物中一样。然而,年龄较大的动物表现出有利于 G2A 同种型的偏向,这表明尽管在主要库生成期间 G2A 和 G2B 的重排是随机启动的,但两个非常相似的 IgM 序列似乎随着年龄和对 Ag 的暴露而表现出不同的表达。我们对免疫个体的 B 细胞进行了基因组单细胞 PCR,以研究激活诱导的胞嘧啶脱氨酶靶向,发现超突变,就像 V(D)J 重排一样,在许多鲨鱼 IgH 中独立发生。

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