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本文引用的文献

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A role of Dishevelled in relocating Axin to the plasma membrane during wingless signaling.在无翅信号传导过程中,散乱蛋白在将轴蛋白重新定位到质膜上的作用。
Curr Biol. 2003 May 27;13(11):960-6. doi: 10.1016/s0960-9822(03)00370-1.
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p53 has a direct apoptogenic role at the mitochondria.p53在线粒体中具有直接的促凋亡作用。
Mol Cell. 2003 Mar;11(3):577-90. doi: 10.1016/s1097-2765(03)00050-9.
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Armadillo/beta-catenin signals in the nucleus--proof beyond a reasonable doubt?犰狳蛋白/β-连环蛋白在细胞核中的信号传导——确凿无疑的证据?
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Wg/Wnt signal can be transmitted through arrow/LRP5,6 and Axin independently of Zw3/Gsk3beta activity.Wg/Wnt信号可独立于Zw3/Gsk3β活性,通过箭蛋白/LRP5、6和Axin进行传递。
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Axin-mediated CKI phosphorylation of beta-catenin at Ser 45: a molecular switch for the Wnt pathway.轴蛋白介导的β-连环蛋白第45位丝氨酸的酪蛋白激酶I磷酸化:Wnt信号通路的分子开关
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Expression and characterization of GSK-3 mutants and their effect on beta-catenin phosphorylation in intact cells.GSK-3突变体的表达、特性及其对完整细胞中β-连环蛋白磷酸化的影响
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GSK-3 inhibition by adenoviral FRAT1 overexpression is neuroprotective and induces Tau dephosphorylation and beta-catenin stabilisation without elevation of glycogen synthase activity.通过腺病毒介导的FRAT1过表达抑制GSK-3具有神经保护作用,并能诱导Tau去磷酸化和β-连环蛋白稳定,而不会提高糖原合酶活性。
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靶向不同亚细胞区室的β-连环蛋白的信号传导活性。

Signalling activity of beta-catenin targeted to different subcellular compartments.

作者信息

Hagen Thilo, Sethi Jaswinder K, Foxwell Neale, Vidal-Puig Antonio

机构信息

Wolfson Digestive Diseases Centre, University Hospital, Nottingham NG7 2UH, UK.

出版信息

Biochem J. 2004 Apr 15;379(Pt 2):471-7. doi: 10.1042/BJ20031749.

DOI:10.1042/BJ20031749
PMID:14733614
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1224088/
Abstract

Beta-catenin plays a dual role as an adhesion molecule in adherens junctions at the plasma membrane and as a key intermediate in the canonical Wnt signalling pathway. The cytosolic soluble pool of beta-catenin, involved in the transmission of the Wnt signal, is normally subjected to rapid protein degradation. On activation of the Wnt cascade, beta-catenin becomes stabilized and then translocates into the nucleus where it co-activates transcription factors of the TCF (T-cell factor)/LEF (lymphoid enhancer factor) family. The expression of plasma membrane-targeted forms of beta-catenin has been shown to also activate TCF/LEF-dependent transcription and different mechanisms have been put forward. In the present study, we have undertaken a systematic analysis of the signalling capability of non-degradable forms of beta-catenin targeted to different cellular compartments. beta-Catenin targeted to the plasma membrane activated transcription to a greater extent compared with non-targeted beta-catenin, and led to a marked stabilization of cytosolic soluble beta-catenin. These effects were independent of the competition with endogenous beta-catenin for binding to E-cadherin at the plasma membrane, since targeting non-degradable beta-catenin to other cellular compartments, i.e. the outer mitochondrial membrane and the endoplasmic reticulum membrane, also resulted in the accumulation of cytosolic wild-type beta-catenin and activation of beta-catenin-dependent signalling. In contrast, nuclear-targeted beta-catenin was without significant effect on cytosolic wild-type beta-catenin and did not activate transcription. Our results suggest that cytosolic accumulation of beta-catenin is a prerequisite for the activation of TCF/LEF-dependent transcription in the nucleus.

摘要

β-连环蛋白在质膜的黏着连接中作为一种黏附分子发挥双重作用,同时也是经典Wnt信号通路中的关键中间体。参与Wnt信号传递的胞质可溶性β-连环蛋白池通常会经历快速的蛋白质降解。在Wnt级联反应激活时,β-连环蛋白变得稳定,然后转运到细胞核中,在那里它与TCF(T细胞因子)/LEF(淋巴样增强因子)家族的转录因子共同激活转录。已证明靶向质膜的β-连环蛋白形式的表达也能激活TCF/LEF依赖的转录,并提出了不同的机制。在本研究中,我们对靶向不同细胞区室的不可降解形式的β-连环蛋白的信号传导能力进行了系统分析。与未靶向的β-连环蛋白相比,靶向质膜的β-连环蛋白在更大程度上激活转录,并导致胞质可溶性β-连环蛋白的显著稳定。这些效应独立于与内源性β-连环蛋白在质膜上结合E-钙黏着蛋白的竞争,因为将不可降解的β-连环蛋白靶向其他细胞区室,即线粒体外膜和内质网膜,也会导致胞质野生型β-连环蛋白的积累和β-连环蛋白依赖信号的激活。相反,靶向细胞核的β-连环蛋白对胞质野生型β-连环蛋白没有显著影响,也不激活转录。我们的结果表明,β-连环蛋白在胞质中的积累是激活细胞核中TCF/LEF依赖转录的先决条件。