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首页> 外文期刊>Mechanisms of Development >BCL9-2 binds Arm/beta-catenin in a Tyr142-independent manner and requires Pygopus for its function in Wg/Wnt signaling
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BCL9-2 binds Arm/beta-catenin in a Tyr142-independent manner and requires Pygopus for its function in Wg/Wnt signaling

机译:BCL9-2以不依赖Tyr142的方式结合Arm / beta-catenin,并需要Pygopu​​s发挥其在Wg / Wnt信号传导中的功能

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摘要

The Wingless (Wg)/Wnt signal transduction pathway controls fundamental processes during animal development. Deregulation of the Wg/Wnt pathway has been causally linked to several forms of cancer, most notably to colorectal cancer. In response to Wg/Wnt signaling, Armadillo/beta-catenin associates in the nucleus with DNA bound TCF and several co-factors, among them Legless/BCL9, which provides a link to Pygopus. Recently, the second vertebrate homologue of Legless, BCL9-2 (or B9L), was characterized and proposed to mediate Wnt signaling in a Pygopus-independent manner, by binding to a Tyrosine-142-phosphorylated form of beta-catenin. Here we examine the role of Tyrosine-142 phosphorylation in several assays and find that it is neither important for the recruitment of BCL9-2, nor for the transcriptional activity of beta-catenin in cultured mammalian cells, nor in Drosophila for Wg signaling activity in vivo. Furthermore, we demonstrate that BCL9-2 can functionally replace Lgs both in cultured cells as well as in vivo and that this rescue activity depends on the ability of BCL9-2 to bind Pygo. Our results do not show a significant functional difference between BCL9-2 and BCL9 but rather suggest that the two proteins represent evolutionary duplicates of Legless, which have acquired distinct expression patterns while acting in a largely redundant manner.
机译:Wingless(Wg)/ Wnt信号转导途径控制着动物发育过程中的基本过程。 Wg / Wnt通路的失调与癌症的几种形式有因果关系,最明显的是与大肠癌有关。作为对Wg / Wnt信号的响应,犰狳/β-catenin在细胞核中与结合DNA的TCF和一些辅助因子(其中包括Legless / BCL9)相关联,从而提供了与侏儒的联系。近来,无腿的第二个脊椎动物同源物BCL9-2(或B9L)的特征和提出是通过与酪氨酸142磷酸化的β-catenin结合,以不依赖于侏儒的方式介导Wnt信号传导。在这里,我们研究了酪氨酸142磷酸化在几种测定中的作用,发现它对BCL9-2的募集,培养的哺乳动物细胞中β-catenin的转录活性以及果蝇中Wg信号转导活性都不重要。体内。此外,我们证明BCL9-2可以在功能上替代培养细胞以及体内的Lgs,并且这种拯救活性取决于BCL9-2结合Pygo的能力。我们的结果并未显示BCL9-2和BCL9之间的显着功能差异,而是表明这两种蛋白代表了Legless的进化复制品,它们获得了明显的表达模式,同时以很大程度上冗余的方式起作用。

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