神经形成
生物
神经管
遗传学
无脑
前脑
神经管缺损
Hox基因
畸形学
基因
胚胎干细胞
转录因子
胚胎
胎儿
原肠化
怀孕
作者
Youssef A. Kousa,Huiping Zhu,Walid D. Fakhouri,Yunping Lei,Akira Kinoshita,Raeuf Roushangar,Nicole Patel,A. J. Agopian,Wei Yang,Elizabeth J. Leslie,Tamara Busch,Tamer Mansour,Xiao Li,Arianna Smith,Edward B. Li,Dhruv Sharma,Trevor J Williams,Yang Chai,Brad A. Amendt,Eric C. Liao
摘要
Mutations in IRF6, TFAP2A and GRHL3 cause orofacial clefting syndromes in humans. However, Tfap2a and Grhl3 are also required for neurulation in mice. Here, we found that homeostasis of Irf6 is also required for development of the neural tube and associated structures. Over-expression of Irf6 caused exencephaly, a rostral neural tube defect, through suppression of Tfap2a and Grhl3 expression. Conversely, loss of Irf6 function caused a curly tail and coincided with a reduction of Tfap2a and Grhl3 expression in tail tissues. To test whether Irf6 function in neurulation was conserved, we sequenced samples obtained from human cases of spina bifida and anencephaly. We found two likely disease-causing variants in two samples from patients with spina bifida. Overall, these data suggest that the Tfap2a-Irf6-Grhl3 genetic pathway is shared by two embryologically distinct morphogenetic events that previously were considered independent during mammalian development. In addition, these data suggest new candidates to delineate the genetic architecture of neural tube defects and new therapeutic targets to prevent this common birth defect.
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