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楔齿蜥(Sphenodon punctatus)主要组织相容性复合体I类基因座的两种变异模式。

Two patterns of variation among MHC class I loci in Tuatara (Sphenodon punctatus).

作者信息

Miller Hilary C, Andrews-Cookson Matiu, Daugherty Charles H

机构信息

Allan Wilson Centre for Molecular Ecology and Evolution, School of Biological Sciences, Victoria University of Wellington, PO Box 600, Wellington, 6140 New Zealand.

出版信息

J Hered. 2007 Nov-Dec;98(7):666-77. doi: 10.1093/jhered/esm095. Epub 2007 Nov 21.

Abstract

The genes of the major histocompatibility complex (MHC) are a central component of the immune system in vertebrates and have become important markers of functional, fitness-related genetic variation. We have investigated the evolutionary processes that generate diversity at MHC class I genes in a large population of an archaic reptile species, the tuatara (Sphenodon punctatus), found on Stephens Island, Cook Strait, New Zealand. We identified at least 2 highly polymorphic (UA type) loci and one locus (UZ) exhibiting low polymorphism. The UZ locus is characterized by low nucleotide diversity and weak balancing selection and may be either a nonclassical class I gene or a pseudogene. In contrast, the UA-type alleles have high nucleotide diversity and show evidence of balancing selection at putative peptide-binding sites. Twenty-one different UA-type genotypes were identified among 26 individuals, suggesting that the Stephens Island population has high levels of MHC class I variation. UA-type allelic diversity is generated by a mixture of point mutation and gene conversion. As has been found in birds and fish, gene conversion obscures the genealogical relationships among alleles and prevents the assignment of alleles to loci. Our results suggest that the molecular mechanisms that underpin MHC evolution in nonmammals make locus-specific amplification impossible in some species.

摘要

主要组织相容性复合体(MHC)基因是脊椎动物免疫系统的核心组成部分,已成为功能性、与适应性相关的遗传变异的重要标记。我们研究了在新西兰库克海峡斯蒂芬斯岛上发现的一种古老爬行动物——喙头蜥(Sphenodon punctatus)的大量种群中,MHC I类基因产生多样性的进化过程。我们鉴定出至少2个高度多态的(UA型)位点和1个表现出低多态性的位点(UZ)。UZ位点的特征是核苷酸多样性低且平衡选择较弱,可能是一个非经典的I类基因或假基因。相比之下,UA型等位基因具有较高的核苷酸多样性,并在假定的肽结合位点显示出平衡选择的证据。在26个个体中鉴定出21种不同的UA型基因型,这表明斯蒂芬斯岛种群具有高水平的MHC I类变异。UA型等位基因多样性是由点突变和基因转换共同产生的。正如在鸟类和鱼类中所发现的那样,基因转换模糊了等位基因之间的谱系关系,并阻止了将等位基因分配到特定位点。我们的结果表明,非哺乳动物中支撑MHC进化的分子机制使得在某些物种中进行位点特异性扩增成为不可能。

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