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HMG盒转录因子SoxNeuro与Tcf共同作用以控制Wg/Wnt信号活性。

The HMG-box transcription factor SoxNeuro acts with Tcf to control Wg/Wnt signaling activity.

作者信息

Chao Anna T, Jones Whitney M, Bejsovec Amy

机构信息

Department of Biology, Duke University, Durham, NC 27708, USA.

出版信息

Development. 2007 Mar;134(5):989-97. doi: 10.1242/dev.02796. Epub 2007 Jan 31.

Abstract

Wnt signaling specifies cell fates in many tissues during vertebrate and invertebrate embryogenesis. To understand better how Wnt signaling is regulated during development, we have performed genetic screens to isolate mutations that suppress or enhance mutations in the fly Wnt homolog, wingless (wg). We find that loss-of-function mutations in the neural determinant SoxNeuro (also known as Sox-neuro, SoxN) partially suppress wg mutant pattern defects. SoxN encodes a HMG-box-containing protein related to the vertebrate Sox1, Sox2 and Sox3 proteins, which have been implicated in patterning events in the early mouse embryo. In Drosophila, SoxN has previously been shown to specify neural progenitors in the embryonic central nervous system. Here, we show that SoxN negatively regulates Wg pathway activity in the embryonic epidermis. Loss of SoxN function hyperactivates the Wg pathway, whereas its overexpression represses pathway activity. Epistasis analysis with other components of the Wg pathway places SoxN at the level of the transcription factor Pan (also known as Lef, Tcf) in regulating target gene expression. In human cell culture assays, SoxN represses Tcf-responsive reporter expression, indicating that the fly gene product can interact with mammalian Wnt pathway components. In both flies and in human cells, SoxN repression is potentiated by adding ectopic Tcf, suggesting that SoxN interacts with the repressor form of Tcf to influence Wg/Wnt target gene transcription.

摘要

在脊椎动物和无脊椎动物胚胎发育过程中,Wnt信号通路决定了许多组织中的细胞命运。为了更好地理解Wnt信号通路在发育过程中是如何被调控的,我们进行了遗传筛选,以分离出抑制或增强果蝇Wnt同源基因无翅(wg)突变的突变体。我们发现,神经决定因子SoxNeuro(也称为Sox-neuro、SoxN)的功能丧失突变部分抑制了wg突变体的模式缺陷。SoxN编码一种含有HMG盒的蛋白质,与脊椎动物的Sox1、Sox2和Sox3蛋白质相关,这些蛋白质与小鼠早期胚胎的模式形成事件有关。在果蝇中,先前已证明SoxN可确定胚胎中枢神经系统中的神经祖细胞。在这里,我们表明SoxN在胚胎表皮中负调控Wg信号通路的活性。SoxN功能的丧失会过度激活Wg信号通路,而其过表达则会抑制信号通路的活性。与Wg信号通路其他成分的上位性分析表明,在调节靶基因表达方面,SoxN作用于转录因子Pan(也称为Lef、Tcf)水平。在人类细胞培养试验中,SoxN抑制Tcf反应性报告基因的表达,表明果蝇基因产物可与哺乳动物Wnt信号通路成分相互作用。在果蝇和人类细胞中,添加异位Tcf均可增强SoxN的抑制作用,这表明SoxN与Tcf的抑制形式相互作用,以影响Wg/Wnt靶基因的转录。

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