先证者
生物
遗传学
外显子组测序
心脏病
外显子组
突变
法洛四联症
基因
内科学
医学
作者
Sheng Chih Jin,Jason Homsy,Samir Zaidi,Qiongshi Lu,Sarah U. Morton,Steven R. DePalma,Xue Zeng,Hongjian Qi,Wen-I Chang,Michael C. Sierant,Wei-Chien Hung,Shozeb Haider,Junhui Zhang,James Knight,Robert Bjornson,Christopher Castaldi,Irina R Tikhonoa,Kaya Bilgüvar,Shrikant Mane,Stephan Sanders
出处
期刊:Nature Genetics
[Nature Portfolio]
日期:2017-10-09
卷期号:49 (11): 1593-1601
被引量:881
摘要
Congenital heart disease (CHD) is the leading cause of mortality from birth defects. Here, exome sequencing of a single cohort of 2,871 CHD probands, including 2,645 parent-offspring trios, implicated rare inherited mutations in 1.8%, including a recessive founder mutation in GDF1 accounting for ∼5% of severe CHD in Ashkenazim, recessive genotypes in MYH6 accounting for ∼11% of Shone complex, and dominant FLT4 mutations accounting for 2.3% of Tetralogy of Fallot. De novo mutations (DNMs) accounted for 8% of cases, including ∼3% of isolated CHD patients and ∼28% with both neurodevelopmental and extra-cardiac congenital anomalies. Seven genes surpassed thresholds for genome-wide significance, and 12 genes not previously implicated in CHD had >70% probability of being disease related. DNMs in ∼440 genes were inferred to contribute to CHD. Striking overlap between genes with damaging DNMs in probands with CHD and autism was also found.
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