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哺乳动物MHC基因中多态性等位基因的位点特异性及生死过程驱动的进化

Locus specificity of polymorphic alleles and evolution by a birth-and-death process in mammalian MHC genes.

作者信息

Gu X, Nei M

机构信息

Institute of Molecular Evolutionary Genetics, Pennsylvania State University, USA.

出版信息

Mol Biol Evol. 1999 Feb;16(2):147-56. doi: 10.1093/oxfordjournals.molbev.a026097.

DOI:10.1093/oxfordjournals.molbev.a026097
PMID:10028282
Abstract

We have conducted an extensive phylogenetic analysis of polymorphic alleles from human and mouse major histocompatibility complex (MHC) class I and class II genes. The phylogenetic tree obtained for 212 complete human class I allele sequences (HLA-A, -B, and -C) has shown that all alleles from the same locus form a single cluster, which is highly supported by bootstrap values, except for one HLA-B allele (HLA-B*7301). Mouse MHC class I loci did not show locus-specific clusters of polymorphic alleles. This was considered to be because of either interlocus genetic exchange or the confusing designation of loci in different haplotypes at the present time. The locus specificity of polymorphic alleles was also observed in human and mouse MHC class II loci. It was therefore concluded that interlocus recombination or gene conversion is not very important for generating MHC diversity, with a possible exception of mouse class I loci. According to the phylogenetic trees of complete coding sequences, we classified human MHC class I (HLA-A, -B, and -C) and class II (DRB1) alleles into three to five major allelic lineages (groups), which were monophyletic with high bootstrap values. Most of these allelic groups remained unchanged even in phylogenetic trees based on individual exons, though this does not exclude the possibility of intralocus recombination involving short DNA segments. These results, together with the previous observation that MHC loci are subject to frequent duplication and deletion, as well as to balancing selection, indicate that MHC evolution in mammals is in agreement with the birth-and-death model of evolution, rather than with the model of concerted evolution.

摘要

我们对人类和小鼠主要组织相容性复合体(MHC)I类和II类基因的多态性等位基因进行了广泛的系统发育分析。从212条完整的人类I类等位基因序列(HLA-A、-B和-C)获得的系统发育树表明,来自同一基因座的所有等位基因形成一个单一的簇,除了一个HLA-B等位基因(HLA-B*7301)外,该簇得到了自展值的高度支持。小鼠MHC I类基因座未显示多态性等位基因的基因座特异性簇。这被认为是由于基因座间的遗传交换或目前不同单倍型中基因座命名的混淆。在人类和小鼠MHC II类基因座中也观察到了多态性等位基因的基因座特异性。因此得出结论,基因座间重组或基因转换对于产生MHC多样性不是非常重要,小鼠I类基因座可能是个例外。根据完整编码序列的系统发育树,我们将人类MHC I类(HLA-A、-B和-C)和II类(DRB1)等位基因分为三到五个主要等位基因谱系(组),这些谱系在高自展值下是单系的。即使在基于单个外显子的系统发育树中,这些等位基因组中的大多数也保持不变,尽管这并不排除涉及短DNA片段的基因座内重组的可能性。这些结果,连同先前观察到的MHC基因座频繁发生重复和缺失以及平衡选择,表明哺乳动物中的MHC进化符合进化的生死模型,而不是协同进化模型。

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