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Novel insights into the genetic landscape of congenital heart disease with systems genetics

机译:具有系统遗传学对先天性心脏病遗传景观的小说洞察

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We recently conducted a large-scale mouse mutagenesis screen and uncovered a central role for cilia in the pathogenesis of congenital heart disease (CHD). Though our screen was phenotype based, most of the genes recovered were cilia-related, including genes encoding proteins important for ciliogenesis, cilia-transduced cell signaling, and vesicular trafficking. Also unexpected, many of the cilia related genes recovered are known direct protein-protein interactors, even though each gene was recovered independently in unrelated mouse lines. These findings suggest a cilia-based protein-protein interactome network may provide the context for congenital heart disease pathogenesis. This could explain the incomplete penetrance and variable expressivity of human CHD, and account for its complex non-Mendelian etiology. Supporting these findings in mice, a preponderance of cilia and cilia related cell signaling genes were observed among de novo pathogenic variants identified in a CHD patient cohort. Further clinical relevance unfolded with the observation of a high prevalence of respiratory cilia dysfunction in CHD patients. This was associated with increased postsurgical respiratory complications. Together these findings highlight the importance of cilia in CHD pathogenesis and suggest possible clinical translation with instituting pulmonary therapy to improve outcome for CHD patients undergoing congenital cardiac surgeries.
机译:我们最近进行了大规模的小鼠诱变筛网​​,并发现了在先天性心脏病(CHD)的发病机制中对纤毛的核心作用。虽然我们的筛选是基于表型的,但是恢复的大多数基因是纤毛相关的,包括编码蛋白质的基因对于纤氯,纤毛转导的细胞信号传导和囊泡贩运。同样出乎意料的是,回收的许多纤毛相关基因是已知的直接蛋白质 - 蛋白互动剂,即使每个基因在不相关的小鼠线中独立回收。这些发现表明基于纤毛的蛋白质 - 蛋白质蛋白联蛋白核集网络可以为先天性心脏病发病机制提供上下文。这可以解释人类CHD的不完全渗透率和可变的表达性,并且占其复杂的非孟德梅的病因。在CHD患者队列中鉴定的De Novo致病变体中,观察到患小鼠的这些发现,纤毛和纤毛相关细胞信号传导基因的优势。通过观察CHD患者呼吸纤毛功能障碍的高患病率展开的进一步临床相关性。这与后期后呼吸道并发症增加有关。这些研究结果共同突出了纤毛在CHD发病机制中的重要性,并提出了在进行肺部治疗的可能临床翻译,以改善接受先天性心脏病患者的CHD患者的结果。

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