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The interplay of genetic and environmental factors in craniofacial morphogenesis: holoprosencephaly and the role of cholesterol.

机译:颅面形态发生中遗传因素和环境因素的相互作用:全前脑和胆固醇的作用。

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摘要

Cyclopia, the paradigmatic "face [that] predicts the brain" in severe holoprosencephaly (HPE) (DeMyer et al., 1964), has been recognized since ancient times. Descriptive embryologists and pathologists have noted the continuum of defective separation of the forebrain and loss of central nervous system (CNS) midline structures for more than a century. It has been recognized more recently that inhibitors of cholesterol biosynthesis, whether consumed in native plants by range sheep, or experimentally applied to early embryos, could phenocopy the natural malformation, as could a variety of other teratogens (maternal diabetes, alcohol). Yet it has been less than a decade that the genomic knowledge base and powerful analytic methods have brought the sciences of descriptive, molecular, and genetic embryology within range of each other. In this review, we discuss the clinical presentations and pathogenesis of HPE. We will outline various genetic and teratogenic mechanisms leading to HPE. Lastly, we will attemptto examine the pivotal role of cholesterol and the Sonic Hedgehog (Shh) pathway in this disorder and in normal embryonic forebraindevelopment.
机译:Cyclopia是严重全脑性前脑(HPE)的典型“预测大脑的面孔”(DeMyer等,1964),自古以来就已被认可。描述性胚胎学家和病理学家已经注意到,前脑的缺陷分离和中枢神经系统(CNS)中线结构丧失的连续性是一个多世纪。最近已经认识到,无论是放牧绵羊在本地植物中消耗的胆固醇生物合成抑制剂,还是实验性应用于早期胚胎的胆固醇生物合成抑制剂,都可以表象自然畸形,其他多种致畸物(母体糖尿病,酒精)也可以。然而,不到不到十年的时间,基因组学知识基础和强大的分析方法就将描述性,分子和遗传胚胎学的科学彼此融合在一起。在这篇综述中,我们讨论了HPE的临床表现和发病机理。我们将概述导致HPE的各种遗传和致畸机制。最后,我们将尝试检查胆固醇和Sonic Hedgehog(Shh)途径在这种疾病和正常胚胎前脑发育中的关键作用。

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