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FGF - 4增强子的发育特异性活性需要Sox2和Oct - 3的协同作用。

Developmental-specific activity of the FGF-4 enhancer requires the synergistic action of Sox2 and Oct-3.

作者信息

Yuan H, Corbi N, Basilico C, Dailey L

机构信息

Department of Microbiology, New York University School of Medicine, New York 10016, USA.

出版信息

Genes Dev. 1995 Nov 1;9(21):2635-45. doi: 10.1101/gad.9.21.2635.

Abstract

Fibroblast growth factor 4 (FGF-4) has been shown to be a signaling molecule whose expression is essential for postimplantation mouse development and, at later embryonic stages, for limb patterning and growth. The FGF-4 gene is expressed in the blastocyst inner cell mass and later in distinct embryonic tissues but is transcriptionally silent in the adult. In tissue culture FGF-4 expression is restricted to undifferentiated embryonic stem (ES) cells and embryonal carcinoma (EC) cell lines. Previously, we determined that EC cell-specific transcriptional activation of the FGF-4 gene depends on a synergistic interaction between octamer-binding proteins and an EC-specific factor, Fx, that bind adjacent sites on the FGF-4 enhancer. Through the cloning and characterization of an F9 cell cDNA we now show that the latter activity is Sox2, a member of the Sry-related Sox factors family. Sox2 can form a ternary complex with either the ubiquitous Oct-1 or the embryonic-specific Oct-3 protein on FGF-4 enhancer DNA sequences. However, only the Sox2/Oct-3 complex is able to promote transcriptional activation. These findings identify FGF-4 as the first known embryonic target gene for Oct-3 and for any of the Sox factors, and offer insights into the mechanisms of selective gene activation by Sox and octamer-binding proteins during embryogenesis.

摘要

成纤维细胞生长因子4(FGF - 4)已被证明是一种信号分子,其表达对于植入后小鼠发育至关重要,并且在胚胎后期对于肢体模式形成和生长也至关重要。FGF - 4基因在囊胚内细胞团中表达,随后在不同的胚胎组织中表达,但在成体中处于转录沉默状态。在组织培养中,FGF - 4的表达仅限于未分化的胚胎干细胞(ES)和胚胎癌细胞(EC)系。此前,我们确定FGF - 4基因的EC细胞特异性转录激活取决于八聚体结合蛋白与一种EC特异性因子Fx之间的协同相互作用,它们结合在FGF - 4增强子的相邻位点上。通过对F9细胞cDNA的克隆和表征,我们现在表明后一种活性是Sox2,它是Sry相关Sox因子家族的成员。Sox2可以与FGF - 4增强子DNA序列上普遍存在的Oct - 1或胚胎特异性的Oct - 3蛋白形成三元复合物。然而,只有Sox2/Oct - 3复合物能够促进转录激活。这些发现确定FGF - 4是Oct - 3以及任何Sox因子的第一个已知胚胎靶基因,并为胚胎发生过程中Sox和八聚体结合蛋白选择性基因激活的机制提供了见解。

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