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首页> 外文期刊>Molecular ecology >Nonparallelism in MHCIIβ diversity accompanies nonparallelism in pathogen infection of lake whitefish (Coregonus clupeaformis) species pairs as revealed by next-generation sequencing
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Nonparallelism in MHCIIβ diversity accompanies nonparallelism in pathogen infection of lake whitefish (Coregonus clupeaformis) species pairs as revealed by next-generation sequencing

机译:下一代测序显示,MHCIIβ多样性的不平行伴随着湖白鱼(Coregonus clupeaformis)物种对的病原体感染。

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Major histocompatibility (MHC) immune system genes may evolve in response to pathogens in the environment. Because they also may affect mate choice, they are candidates for having great importance in ecological speciation. Here, we use next-generation sequencing to test the general hypothesis of parallelism in patterns of MHCIIβ diversity and bacterial infections among five dwarf and normal whitefish sympatric pairs. A second objective was to assess the functional relationships between specific MHCIIβ alleles and pathogens in natural conditions. Each individual had between one and four alleles, indicating two paralogous loci. In Cliff Lake, the dwarf ecotype was monomorphic for the most common allele. In Webster Lake, the skew in the allelic distribution was towards the same allele but in the normal ecotype, underscoring the nonparallel divergence among lakes. Our signal of balancing selection matched putative peptide binding region residues in some cases, but not in others, supporting other recent findings of substantial functional differences in fish MHCIIβ compared with mammals. Individuals with fewer alleles were less likely to be infected; thus, we found no evidence for the heterozygote advantage hypothesis. MHCIIβ alleles and pathogenic bacteria formed distinct clusters in multivariate analyses, and clusters of certain alleles were associated with clusters of pathogens, or sometimes the absence of pathogens, indicating functional relationships at the individual level. Given that patterns of MHCIIβ and bacteria were nonparallel among dwarf and normal whitefish pairs, we conclude that pathogens driving MHCIIβ evolution did not play a direct role in their parallel phenotypic evolution.
机译:主要组织相容性(MHC)免疫系统基因可能会响应环境中的病原体而进化。由于它们也可能影响配偶的选择,因此它们在生态物种形成中非常重要。在这里,我们使用下一代测序来检验MHCIIβ多样性和五个白矮星和正常白鲑同胞对中细菌感染的平行性的一般假设。第二个目标是评估自然条件下特定MHCIIβ等位基因与病原体之间的功能关系。每个个体具有一到四个等位基因,表明两个旁系基因座。在悬崖湖中,侏儒生态型对于最常见的等位基因是单态的。在韦伯斯特湖中,等位基因分布的偏斜朝向相同的等位基因,但在正常生态型中偏斜,这突出了各湖之间非平行的差异。我们的平衡选择信号在某些情况下与推定的肽结合区残基匹配,但在其他情况下却不匹配,这支持了鱼类MHCIIβ与哺乳动物相比在功能上存在实质性差异的其他最新发现。等位基因较少的个体被感染的可能性较小;因此,我们没有发现杂合子优势假说的证据。 MHCIIβ等位基因和致病菌在多变量分析中形成了独特的簇,某些等位基因的簇与病原体簇相关,有时甚至没有病原体,表明了个体水平的功能关系。考虑到MHCIIβ和细菌的模式在侏儒和正常白鲑对之间是不平行的,我们得出的结论是,驱动MHCIIβ进化的病原体在其平行表型进化中没有直接作用。

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