缺氧会阻碍颅神经嵴细胞分化成与颅面发育有关的衍生物

Theresa Schmid, Gabriele Rodrian, Alexander Kohler, Michael Wegner, Lina Goelz, Matthias Weider
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引用次数: 0

摘要

口面裂隙是第二大最常见的先天性畸形。风险因素是多方面的,包括遗传因素和环境因素。环境因素之一是孕期缺氧,例如吸烟、药物或生活在高海拔地区。人们对缺氧与口面裂隙之间的分子联系了解甚少。我们在此表明,缺氧对增殖中的颅神经嵴细胞影响不大,但却极大地影响了它们的分化潜能。我们检测到它们向软骨细胞、成骨细胞和平滑肌细胞分化的过程受到了严重干扰。全基因组转录组分析表明,缺氧条件严重影响了这些过程中大多数受调控基因的转录诱导。生物信息学分析表明,细胞骨架组织和氨基酸代谢是所有三个分化途径中受到损害的两个主要过程,缺氧条件下诱导受损的基因中还包括几个口裂风险基因。我们的分析揭示了缺氧对颅骨神经嵴细胞分化潜能的巨大影响,这可能是口面裂发生的根源。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Hypoxia impedes differentiation of cranial neural crest cells into derivatives relevant for craniofacial development
Orofacial clefts are the second-most prevalent congenital malformation. Risk factors are multifactorial and include genetic components but also environmental factors. One environmental factor is hypoxia during pregnancy, caused for instance by tobacco smoking, medication or living at high altitudes. Knowledge about the molecular link between hypoxia and orofacial clefts is at large. We here show that hypoxia has only modest effects on proliferating cranial neural crest cells, but dramatically influences their differentiation potential. We detected massive perturbations in their differentiation to chondrocytes, osteoblasts and smooth muscle cells. The transcriptional induction of the majority of regulated genes during each of these processes was grossly impaired by hypoxic conditions, as evidenced by genome-wide transcriptomic analyses. Bioinformatic analyses pointed to cytoskeletal organization and amino acid metabolism as two main processes compromised during all three differentiation pathways, and several orofacial cleft risk genes were among the genes with impaired induction during hypoxia. Our analyses reveal a drastic influence of hypoxia on the differentiation potential of cranial neural crest cells as a possible source for the occurrence of orofacial clefts.
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