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HLA-A、B、C等位基因的多样性与多样化

Diversity and diversification of HLA-A,B,C alleles.

作者信息

Parham P, Lawlor D A, Lomen C E, Ennis P D

机构信息

Department of Cell Biology, Stanford University, CA 94305.

出版信息

J Immunol. 1989 Jun 1;142(11):3937-50.

PMID:2715640
Abstract

The nucleotide sequences encoding 14 HLA-A,B,C and 5 ChLA-A,B,C molecules have been determined. Combining these sequences with published data has enabled the polymorphism in 40 HLA-A,B,C and 9 ChLA-A,B,C alleles to be analyzed. Diversity is generated through assortment of point mutations by recombinational mechanisms including gene and allelic conversions. The distribution and frequency of silent and replacement substitutions indicate that there has been positive selection for allelic diversity in the 5' part of the gene (exons 1 to 3) and for allelic homogenization and locus specificity in the 3' part of the gene (exons 4 to 8). These differences may correlate with the lengths of converted sequences in the two parts of the gene and frequency of the CpG dinucleotide. Locus-specific divergence of HLA-A,B, and C demonstrates that recombinational events involving alleles of a locus have been more important than conversion between loci. This contrasts with the predominance of gene conversion events in the evolution of mutants of the H-2Kb gene. However, a striking example of gene conversion involving HLA-B and C alleles of an oriental haplotype has been found. Comparison of human and chimpanzee alleles reveals extensive sharing of polymorphisms, confirming that diversification is a slow process, and that much of contemporary polymorphism originated in ancestral primate species before the emergence of Homo sapiens. There is less polymorphism at the HLA-A locus compared to HLA-B, with greater similarity also being seen between HLA-A and ChLA-A alleles than between HLA-B and ChLA-B alleles. Although greater diversity is seen in the 5' "variable" exons of HLA-B compared to HLA-A, there is increased heterogeneity in the 3' "conserved" exons of HLA-A compared to HLA-B.

摘要

已确定编码14种人类白细胞抗原A、B、C(HLA - A、B、C)分子和5种中国白细胞抗原A、B、C(ChLA - A、B、C)分子的核苷酸序列。将这些序列与已发表的数据相结合,使得能够分析40种HLA - A、B、C等位基因和9种ChLA - A、B、C等位基因中的多态性。多样性是通过包括基因和等位基因转换在内的重组机制对点突变进行分类而产生的。沉默替换和置换替换的分布及频率表明,在基因的5'部分(外显子1至3)存在对等位基因多样性的正选择,而在基因的3'部分(外显子4至8)存在对等位基因同质化和基因座特异性的正选择。这些差异可能与基因两部分中转换序列的长度以及CpG二核苷酸的频率相关。HLA - A、B和C的基因座特异性差异表明,涉及一个基因座等位基因的重组事件比基因座间的转换更为重要。这与H - 2Kb基因突变进化过程中基因转换事件占主导形成对比。然而,已发现一个涉及东方单倍型HLA - B和C等位基因的基因转换的显著例子。人类和黑猩猩等位基因的比较揭示了多态性的广泛共享,证实了多样化是一个缓慢的过程,并且当代的许多多态性起源于智人出现之前的灵长类祖先物种。与HLA - B相比,HLA - A基因座的多态性较少,并且HLA - A和ChLA - A等位基因之间的相似性也高于HLA - B和ChLA - B等位基因之间的相似性。尽管与HLA - A相比,HLA - B的5'“可变”外显子中可见更大的多样性,但与HLA - B相比,HLA - A的3'“保守”外显子中的异质性增加。

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