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紧密连锁的人类白细胞抗原(HLA)基因座之间截然不同的进化史。

Contrasting evolutionary histories among tightly linked HLA loci.

作者信息

Klitz W, Thomson G, Baur M P

出版信息

Am J Hum Genet. 1986 Sep;39(3):340-9.

PMID:3766540
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1683969/
Abstract

Genes comprising the major histocompatibility complex (MHC) play a central role in governing the immune response of vertebrates. A great deal of information has been revealed on the molecular biology and physiology of these loci, but three features-the high polymorphism, tight linkage among the loci, and the nonrandom association of alleles-make the system of particular interest from the perspective of population genetics. Information on the dynamic evolutionary forces that have acted on a locus can be inferred from the number and distribution of alleles that it carries. Ten loci from the HLA region of the human MHC, each sampled from several different populations, have been examined for departures from the expected value of homozygosity under the condition of selective neutrality. The homozygosities of five class I and II loci that code for membrane glycoproteins, HLA-A, -B, -C, -DR, and -DQ, and of glyoxylase I (GLO) were significantly less than the neutrality expectations. This suggests the presence of some form of balancing selection. In spite of being closely linked, in fact, located between the class I and class II histocompatibility loci, the homozygosities of the four class III or complement loci C2, Bf, C4A, and C4B, which are detected by electrophoresis, were indistinguishable from, or exceeded, that expected under neutrality. Although this conforms to the suggestion that, in general, electrophoretic variants are neutral, because of the tight linkage to loci demonstrating a history of selection, it is possible that the mechanism for generating variation in the class III loci may be different from that of the class I and class II loci.

摘要

构成主要组织相容性复合体(MHC)的基因在调控脊椎动物的免疫反应中起着核心作用。关于这些基因座的分子生物学和生理学已经揭示了大量信息,但有三个特征——高度多态性、基因座之间的紧密连锁以及等位基因的非随机关联——使得从群体遗传学的角度来看,这个系统特别引人关注。作用于一个基因座的动态进化力量的信息可以从它所携带的等位基因的数量和分布中推断出来。已经对人类MHC的HLA区域中的10个基因座进行了检测,每个基因座都从几个不同的群体中取样,以检查在选择中性条件下杂合性是否偏离预期值。编码膜糖蛋白的5个I类和II类基因座HLA-A、-B、-C、-DR和-DQ以及乙二醛酶I(GLO)的杂合性显著低于中性预期值。这表明存在某种形式的平衡选择。实际上,尽管四个III类或补体基因座C2、Bf、C4A和C(4)B紧密连锁,位于I类和II类组织相容性基因座之间,但通过电泳检测到的它们的杂合性与中性条件下的预期值没有区别,或者超过了预期值。虽然这符合一般认为电泳变体是中性的观点,但由于与显示有选择历史的基因座紧密连锁,III类基因座产生变异的机制可能与I类和II类基因座不同。

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