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在塑造 MHC 变异中选择和遗传漂变的相对作用。

On the relative roles of selection and genetic drift in shaping MHC variation.

机构信息

Department of Organismic and Evolutionary Biology, Harvard University, Cambridge, MA 02138, USA.

出版信息

Mol Ecol. 2010 Sep;19(18):3842-4. doi: 10.1111/j.1365-294X.2010.04772.x.

Abstract

Genes of the major histocompatibility complex (MHC) have provided some of the clearest examples of how natural selection generates discordances between adaptive and neutral variation in natural populations. The type and intensity of selection as well as the strength of genetic drift are believed to be important in shaping the resulting pattern of MHC diversity. However, evaluating the relative contribution of multiple microevolutionary forces is challenging, and empirical studies have reported contrasting results. For instance, balancing selection has been invoked to explain high levels of MHC diversity and low population differentiation in comparison with other nuclear markers. Other studies have shown that genetic drift can sometimes overcome selection and then patterns of genetic variation at adaptive loci cannot be discerned from those occurring at neutral markers. Both empirical and simulated data also indicate that loss of genetic diversity at adaptive loci can occur faster than at neutral loci when selection and population bottlenecks act simultaneously. Diversifying selection, on the other hand, explains accelerated MHC divergence as the result of spatial variation in pathogen-mediated selective regimes. Because of all these possible scenarios and outcomes, collecting information from as many study systems as possible, is crucial to enhance our understanding about the evolutionary forces driving MHC polymorphism. In this issue, Miller and co-workers present an illuminating contribution by combining neutral markers (microsatellites) and adaptive MHC class I loci during the investigation of genetic differentiation across island populations of tuatara Sphenodon punctatus. Their study of geographical variation reveals a major role of genetic drift in shaping MHC variation, yet they also discuss some support for diversifying selection.

摘要

主要组织相容性复合体 (MHC) 的基因为自然选择如何在自然种群中产生适应性和中性变异之间的不和谐提供了一些最清晰的例子。选择的类型和强度以及遗传漂变的强度被认为是塑造 MHC 多样性的重要因素。然而,评估多种微进化力量的相对贡献具有挑战性,实证研究报告了相互矛盾的结果。例如,平衡选择被认为可以解释 MHC 多样性水平高和与其他核标记相比种群分化程度低的现象。其他研究表明,遗传漂变有时可以克服选择,然后适应性位点的遗传变异模式不能与中性标记的遗传变异模式区分开来。实证和模拟数据还表明,当选择和种群瓶颈同时作用时,适应性位点的遗传多样性损失速度可能比中性位点快。另一方面,多样化选择解释了 MHC 分化的加速,这是由于病原体介导的选择机制在空间上的差异。由于所有这些可能的情况和结果,尽可能多地从研究系统中收集信息对于增强我们对驱动 MHC 多态性的进化力量的理解至关重要。在本期中,Miller 及其同事通过在 Sphenodon punctatus 图阿托拉(tuatara)岛屿种群的遗传分化研究中结合中性标记(微卫星)和适应性 MHC Ⅰ类基因座,提供了一个有启发性的贡献。他们对地理变异的研究揭示了遗传漂变在塑造 MHC 变异方面的主要作用,但他们也讨论了一些支持多样化选择的证据。

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