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Profiling the immunome of little brown myotis provides a yardstick for measuring the genetic response to white‐nose syndrome

机译:对小棕褐鼠的免疫组进行分析为衡量对白鼻综合症的遗传反应提供了衡量标准

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摘要

White‐nose syndrome (WNS) has devastated populations of hibernating bats in eastern North America, leading to emergency conservation listings for several species including the previously ubiquitous little brown myotis (Myotis lucifugus). However, some bat populations near the epicenter of the WNS panzootic appear to be stabilizing after initial precipitous declines, which could reflect a selective immunogenetic sweep. To investigate the hypothesis that WNS exerts significant selection on the immunome of affected bat populations, we developed a novel, high‐throughput sequence capture assay targeting 138 adaptive, intrinsic, and innate immunity genes of putative adaptive significance, as well as their respective regulatory regions (~370 kbp of genomic sequence/individual). We used the assay to explore baseline immunogenetic variation in M. lucifugus and to investigate whether particular immune genes/variants are associated with WNS susceptibility. We also used our assay to detect 1,038 putatively neutral single nucleotide polymorphisms and characterize contemporary population structure, providing context for the identification of local immunogenetic adaptation. Sequence capture provided a cost‐effective, “all‐in‐one” assay to test for neutral genetic and immunogenetic structure and revealed fine‐scale, baseline immunogenetic differentiation between sampling sites <600 km apart. We identified functional immunogenetic variants in M. lucifugus associated with WNS susceptibility. This study lays the foundations for future investigations of rangewide immunogenetic adaptation to WNS in M. lucifugus and provides a blueprint for studies of evolutionary rescue in other host–pathogen systems.
机译:白鼻综合症(WNS)破坏了北美洲东部的冬眠蝙蝠种群,导致包括先前普遍存在的小棕褐Myotis(Myotis lucifugus)在内的几种物种的紧急保护清单。但是,WNS大流行震中附近的一些蝙蝠种群在最初的急剧下降后似乎趋于稳定,这可能反映了选择性的免疫遗传扫描。为了研究WNS在受影响蝙蝠群体的免疫系统中发挥重要选择的假设,我们开发了一种新颖的高通量序列捕获测定法,其针对138个具有公认的自适应意义的适应性,内在和先天免疫基因以及它们各自的调控区域(〜370kbp的基因组序列/个体)。我们使用该测定方法探索了M.lucifugus中的基线免疫遗传变异,并调查了特定的免疫基因/变体是否与WNS易感性相关。我们还使用我们的检测方法来检测1,038个推定的中性单核苷酸多态性并表征当代人群结构,从而为鉴定局部免疫遗传适应性提供了背景。序列捕获提供了一种经济高效的“多合一”测定法来测试中性遗传和免疫遗传结构,并揭示了相距小于600公里的采样点之间的细微基线免疫遗传差异。我们在与WNS易感性相关的M.lucifugus中鉴定了功能性免疫遗传变异体。这项研究为进一步研究在M.lucifugus中对WNS的广泛免疫遗传适应奠定了基础,并为其他宿主-病原体系统中的进化拯救研究提供了蓝图。

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