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TFAP2A-IRF6-GRHL3 基因通路在神经胚形成中保守。

The TFAP2A-IRF6-GRHL3 genetic pathway is conserved in neurulation.

机构信息

Departments of Biochemistry and Molecular Biology.

Division of Neurology, Childrens National Health System.

出版信息

Hum Mol Genet. 2019 May 15;28(10):1726-1737. doi: 10.1093/hmg/ddz010.

DOI:10.1093/hmg/ddz010
PMID:30689861
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6494790/
Abstract

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.

摘要

IRF6、TFAP2A 和 GRHL3 的突变会导致人类的口腔面裂综合征。然而,Tfap2a 和 Grhl3 也对于小鼠的神经胚形成是必需的。在这里,我们发现 Irf6 的内环境平衡对于神经管及其相关结构的发育也是必需的。Irf6 的过表达通过抑制 Tfap2a 和 Grhl3 的表达导致无脑畸形,一种颅神经管缺陷。相反,Irf6 功能的丧失导致卷曲的尾巴,并伴随着尾部组织中 Tfap2a 和 Grhl3 表达的减少。为了测试 Irf6 在神经胚形成中的功能是否保守,我们对来自神经管缺陷(脊柱裂和无脑畸形)患者的样本进行了测序。我们在两个脊柱裂患者的样本中发现了两个可能的致病变异。总的来说,这些数据表明,Tfap2a-Irf6-Grhl3 遗传途径存在于两个胚胎发育上不同的形态发生事件中,这两个事件在哺乳动物发育过程中之前被认为是独立的。此外,这些数据为阐明神经管缺陷的遗传结构提供了新的候选基因,并为预防这种常见的出生缺陷提供了新的治疗靶点。

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