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免疫球蛋白VH基因家族的协同进化。

Concerted evolution of the immunoglobulin VH gene family.

作者信息

Gojobori T, Nei M

机构信息

University of Texas, Houston.

出版信息

Mol Biol Evol. 1984 Feb;1(2):195-212. doi: 10.1093/oxfordjournals.molbev.a040311.

Abstract

With the aim of understanding the concerted evolution of the immunoglobulin VH multigene family, a phylogenetic tree for the DNA sequences of 16 mouse and five human germ line genes was constructed. This tree indicates that all genes in this family have undergone substantial evolutionary divergence. The most closely related genes so far identified in the mouse genome seem to have diverged about 6 million years (MY) ago, whereas the most distantly related genes diverged about 300 MY ago. This suggests that gene duplication caused by unequal crossing-over or gene conversion occurs very slowly in this gene family. The rate of occurrence of gene duplication in the VH gene family has been estimated to be 5 x 10(-7) per gene per year, which seems to be at least about 100 times lower than that for the rRNA gene family. This low rate of concerted evolution in the VH gene family helps retain intergenic genetic variability that in turn contributes to antibody diversity. Because of accumulation of destructive mutations, however, about one-third of the mouse and human VH genes seem to have become nonfunctional. Many of these pseudogenes have apparently originated recently, but some of them seem to have existed in the genome for more than 10 MY. The rate of nucleotide substitution for the complementarity-determining regions (CDRs) is as high as that of pseudogenes. This suggests that there is virtually no purifying selection operating in the CDRs and that germ line mutations are effectively used for generating antibody diversity.

摘要

为了理解免疫球蛋白VH多基因家族的协同进化,构建了16个小鼠和5个人类种系基因DNA序列的系统发育树。该树表明该家族中的所有基因都经历了显著的进化分歧。目前在小鼠基因组中鉴定出的亲缘关系最密切的基因似乎在约600万年前发生了分歧,而亲缘关系最远的基因则在约3亿年前发生了分歧。这表明由不等交换或基因转换引起的基因复制在该基因家族中发生得非常缓慢。VH基因家族中基因复制的发生率估计为每年每个基因5×10⁻⁷,这似乎比rRNA基因家族至少低约100倍。VH基因家族中这种低协同进化速率有助于保留基因间的遗传变异性,进而有助于抗体多样性。然而,由于破坏性突变的积累,约三分之一的小鼠和人类VH基因似乎已失去功能。这些假基因中的许多显然是最近起源的,但其中一些似乎在基因组中已经存在超过1000万年。互补决定区(CDR)的核苷酸替换率与假基因的一样高。这表明在CDR中几乎没有纯化选择起作用,并且种系突变有效地用于产生抗体多样性。

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