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在胚胎早期发育过程中,视黄酸在神经及神经嵴衍生细胞中的饱和积累。

Saturable accumulation of retinoic acid in neural and neural crest derived cells in early embryonic development.

作者信息

Dencker L, d'Argy R, Danielsson B R, Ghantous H, Sperber G O

出版信息

Dev Pharmacol Ther. 1987;10(3):212-23. doi: 10.1159/000457746.

Abstract

Retinoic acid (RA) binds to a cytosolic protein distinguishable from the cellular retinol (R) binding protein. Recent studies, showing an influence by R and RA on genomic expression, suggest an interaction with the cell nucleus mediated by the specific binding proteins in a manner resembling that of steroid hormones. RA can irreversibly stimulate in vitro differentiation of teratocarcinoma cells and support early embryonic development in vitamin A depleted animals. This study demonstrates a saturable, highly specific and regional accumulation of RA in the neuroepithelium and developing CNS that occurs in early but not in late fetal development in the mouse. The results suggest that a binding protein, or some other cellular mechanism for accumulation of RA is expressed in the neural cells only during restricted periods of development. High levels are recorded also in regions where cranial neural crest cells are known to migrate, and later in the visceral arches and maxillary areas, the mesenchyme of which is known to be partly derived from migrating cranial neural crest cells. The specific accumulation of RA in embryonic neural and cranial neural crest cells is in line with animal experiments and human clinical data, showing that retinoids specifically impair CNS, eye, ear, and facial development.

摘要

视黄酸(RA)与一种不同于细胞视黄醇(R)结合蛋白的胞质蛋白结合。最近的研究表明,R和RA对基因组表达有影响,提示它们通过特定结合蛋白与细胞核相互作用,其方式类似于类固醇激素。RA能不可逆地刺激畸胎瘤细胞的体外分化,并支持维生素A缺乏动物的早期胚胎发育。本研究证明,RA在神经上皮和发育中的中枢神经系统中存在可饱和、高度特异性和区域性积累,这种积累发生在小鼠胎儿发育早期而非晚期。结果表明,一种结合蛋白或其他一些积累RA的细胞机制仅在发育的特定时期在神经细胞中表达。在已知颅神经嵴细胞迁移的区域也记录到高水平,随后在内脏弓和上颌区域也有高水平,已知这些区域的间充质部分来源于迁移的颅神经嵴细胞。RA在胚胎神经和颅神经嵴细胞中的特异性积累与动物实验和人类临床数据一致,表明类视黄醇会特异性损害中枢神经系统、眼睛、耳朵和面部发育。

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