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在结构高度复杂的野生大角羊(Ovis dalli)种群中检测免疫基因的选择特征。

Detecting the signature of selection on immune genes in highly structured populations of wild sheep (Ovis dalli).

作者信息

Worley K, Carey J, Veitch A, Coltman D W

机构信息

Department of Animal and Plant Sciences, University of Sheffield, UK.

出版信息

Mol Ecol. 2006 Mar;15(3):623-37. doi: 10.1111/j.1365-294X.2006.02829.x.

Abstract

The confounding effects of population structure complicate efforts to identify regions of the genome under the influence of selection in natural populations. Here we test for evidence of selection in three genes involved in vertebrate immune function - the major histocompatibility complex (MHC), interferon gamma (IFNG) and natural resistance associated macrophage polymorphism (NRAMP) - in highly structured populations of wild thinhorn sheep (Ovis dalli). We examined patterns of variation at microsatellite loci linked to these gene regions and at the DNA sequence level. Simple Watterson's tests indicated balancing selection at all three gene regions. However, evidence for selection was confounded by population structure, as the Watterson's test statistics from linked markers were not outside of the range of values from unlinked and presumably neutral microsatellites. The translated coding sequences of thinhorn IFNG and NRAMP are fixed and identical to those of domestic sheep (Ovis aries). In contrast, the thinhorn MHC DRB locus shows significant evidence of overdominance through both an excess of nonsynonymous substitution and trans-species polymorphism. The failure to detect balancing selection at microsatellite loci linked to the MHC is likely the result of recombination between the markers and expressed gene regions.

摘要

种群结构的混杂效应使得在自然种群中识别受选择影响的基因组区域的工作变得复杂。在此,我们检测了野生细角羊(Ovis dalli)高度结构化种群中涉及脊椎动物免疫功能的三个基因——主要组织相容性复合体(MHC)、干扰素γ(IFNG)和自然抗性相关巨噬细胞多态性(NRAMP)——的选择证据。我们研究了与这些基因区域连锁的微卫星位点以及DNA序列水平上的变异模式。简单的沃特森检验表明这三个基因区域均存在平衡选择。然而,由于种群结构的影响,选择证据变得复杂,因为来自连锁标记的沃特森检验统计量并未超出未连锁且可能为中性的微卫星的取值范围。细角羊IFNG和NRAMP的翻译编码序列是固定的,且与家羊(Ovis aries)的相同。相比之下,细角羊MHC DRB位点通过非同义替换过量和跨物种多态性显示出显著的超显性证据。在与MHC连锁的微卫星位点未能检测到平衡选择,可能是由于标记与表达基因区域之间发生了重组。

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