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首页> 外文期刊>American Journal of Physiology >Genetic determinants of ammonia-induced acute lung injury in mice
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Genetic determinants of ammonia-induced acute lung injury in mice

机译:小鼠氨诱导急性肺损伤的遗传决定因素

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In this study, a genetically diverse panel of 43 mouse strains was exposed to ammonia, and genome-wide association mapping was performed employing a single-nucleotide polymorphism (SNP) assembly. Transcriptomic analysis was used to help resolve the genetic determinants of ammonia-induced acute lung injury. The encoded proteins were prioritized based on molecular function, nonsynony-mous SNP within a functional domain or SNP within the promoter region that altered expression. This integrative functional approach revealed 14 candidate genes that included Aatf, Avil, Cep162, Hrh4, Lama3, Plcb4, and Ube2cbp, which had significant SNP associations, and Aff1, Bcar3, Cntn4, Kcnq5, PrdmiO, Ptcd3, and Snx19, which had suggestive SNP associations. Of these genes, Bcar3, Cep162, Hrh4, Kcnq5, and Lama3 are particularly noteworthy and had pathophysiological roles that could be associated with acute lung injury in several ways.
机译:在这项研究中,43个小鼠品系的遗传多样性小组暴露于氨中,并利用单核苷酸多态性(SNP)组装进行了全基因组关联图谱绘制。转录组学分析用于帮助解决氨诱导急性肺损伤的遗传决定因素。根据分子功能、功能域内的非同义SNP或改变表达的启动子区域内的SNP,对编码的蛋白质进行优先排序。这种综合功能方法揭示了14个候选基因,包括Aatf、Avil、Cep162、Hrh4、Lama3、Plcb4和Ube2cbp,它们具有显著的SNP关联,以及Aff1、Bcar3、Cntn4、Kcnq5、PrdmiO、Ptcd3和Snx19,它们具有提示性SNP关联。在这些基因中,Bcar3、Cep162、Hrh4、Kcnq5和Lama3尤其值得注意,它们具有病理生理作用,可能以多种方式与急性肺损伤相关。

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