Allelic Interaction between CRELD1 and VEGFA in the Pathogenesis of Cardiac Atrioventricular Septal Defects.

Jennifer K Redig, Gameil T Fouad, Darcie Babcock, Benjamin Reshey, Eleanor Feingold, Roger H Reeves, Cheryl L Maslen
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Abstract

Atrioventricular septal defects (AVSD) are highly heritable, clinically significant congenital heart malformations. Genetic and environmental modifiers of risk are thought to work in unknown combinations to cause AVSD. Approximately 5-10% of simplex AVSD cases carry a missense mutation in CRELD1. However, CRELD1 mutations are not fully penetrant and require interactions with other risk factors to result in AVSD. Vascular endothelial growth factor-A (VEGFA) is a well-characterized modulator of heart valve development. A functional VEGFA polymorphism, VEGFA c.-634C, which causes constitutively increased VEGFA expression, has been associated with cardiac septal defects suggesting it may be a genetic risk factor. To determine if there is an allelic association with AVSD we genotyped the VEGFA c.-634 SNP in a simplex AVSD study cohort. Over-representation of the c.-634C allele in the AVSD group suggested that this genotype may increase risk. Correlation of CRELD1 and VEGFA genotypes revealed that potentially pathogenic missense mutations in CRELD1 were always accompanied by the VEGFA c.-634C allele in individuals with AVSD suggesting a potentially pathogenic allelic interaction. We used a Creld1 knockout mouse model to determine the effect of deficiency of Creld1 combined with increased VEGFA on atrioventricular canal development. Morphogenic response to VEGFA was abnormal in Creld1-deficient embryonic hearts, indicating that interaction between CRELD1 and VEGFA has the potential to alter atrioventricular canal morphogenesis. This supports our hypothesis that an additive effect between missense mutations in CRELD1 and a functional SNP in VEGFA contributes to the pathogenesis of AVSD.

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CRELD1和VEGFA在心脏房室间隔缺损发病机制中的基因相互作用
房室间隔缺损(AVSD)是一种遗传性极高、临床意义重大的先天性心脏畸形。遗传和环境因素被认为是导致 AVSD 的未知组合风险因素。约有 5-10% 的单纯性 AVSD 病例携带 CRELD1 的错义突变。然而,CRELD1 基因突变并不具有完全渗透性,需要与其他风险因素相互作用才能导致 AVSD。血管内皮生长因子-A(VEGFA)是一种特征明确的心脏瓣膜发育调节因子。VEGFA c.-634C是一种功能性VEGFA多态性,可导致VEGFA表达的连续性增加,这种多态性与心脏室间隔缺损有关,表明它可能是一种遗传风险因素。为了确定与 AVSD 是否存在等位基因关联,我们在一个单纯性 AVSD 研究队列中对 VEGFA c.-634 SNP 进行了基因分型。在 AVSD 群体中,c.-634C 等位基因的比例过高,这表明该基因型可能会增加风险。CRELD1和VEGFA基因型的相关性显示,在AVSD患者中,CRELD1中潜在的致病性错义突变总是伴随着VEGFA c.-634C等位基因,这表明存在潜在的致病性等位基因相互作用。我们使用 Creld1 基因敲除小鼠模型来确定 Creld1 基因缺失合并 VEGFA 增高对房室管发育的影响。在 Creld1 基因缺陷的胚胎心脏中,VEGFA 的形态发生反应异常,这表明 CRELD1 和 VEGFA 之间的相互作用有可能改变房室管的形态发生。这支持了我们的假设,即 CRELD1 的错义突变和 VEGFA 的功能性 SNP 之间的叠加效应是导致 AVSD 发病的原因。
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AIMS Genetics
AIMS Genetics GENETICS & HEREDITY-
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