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严重的头部发育不良是由于前后发育程序失衡导致的。

Severe head dysgenesis resulting from imbalance between anterior and posterior ontogenetic programs.

机构信息

Université de Strasbourg, Inserm, IRFAC/UMR-S1113, FMTS, 67200, Strasbourg, France.

Karlsruhe Institute of Technology, Institute of Toxicology and Genetics, 76021, Karlsruhe, Germany.

出版信息

Cell Death Dis. 2019 Oct 24;10(11):812. doi: 10.1038/s41419-019-2040-0.

Abstract

Head dysgenesis is a major cause of fetal demise and craniofacial malformation. Although mutations in genes of the head ontogenetic program have been reported, many cases remain unexplained. Head dysgenesis has also been related to trisomy or amplification of the chromosomal region overlapping the CDX2 homeobox gene, a master element of the trunk ontogenetic program. Hence, we investigated the repercussion on head morphogenesis of the imbalance between the head and trunk ontogenetic programs, by means of ectopic rostral expression of CDX2 at gastrulation. This caused severe malformations affecting the forebrain and optic structures, and also the frontonasal process associated with defects in neural crest cells colonization. These malformations are the result of the downregulation of genes of the head program together with the abnormal induction of trunk program genes. Together, these data indicate that the imbalance between the anterior and posterior ontogenetic programs in embryos is a new possible cause of head dysgenesis during human development, linked to defects in setting up anterior neuroectodermal structures.

摘要

头颅发育不全是导致胎儿死亡和颅面畸形的主要原因。虽然已经报道了头发生成程序基因的突变,但许多病例仍无法解释。头颅发育不全也与染色体区域的三倍体或扩增有关,该区域重叠 CDX2 同源盒基因,这是躯干发生程序的主要元素。因此,我们通过在原肠胚期异位表达 CDX2 来研究头发生成程序与躯干发生程序之间的失衡对头部形态发生的影响。这导致了严重的畸形,影响了前脑和视神经结构,以及与神经嵴细胞定植缺陷相关的额鼻突起。这些畸形是头部程序基因下调以及躯干程序基因异常诱导的结果。这些数据表明,胚胎前后发生程序之间的失衡是人类发育过程中头部发育不全的一个新的可能原因,与前神经外胚层结构的建立缺陷有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/685e/6813351/7191b84c0e32/41419_2019_2040_Fig1_HTML.jpg

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