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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >Autophagy and the Wnt signaling pathway: A focus on Wnt/beta-catenin signaling
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Autophagy and the Wnt signaling pathway: A focus on Wnt/beta-catenin signaling

机译:自噬和WNT信令路径:重点是Wnt / beta-catenin信号传导

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摘要

Cellular homeostasis and adaptation to various environmental conditions are importantly regulated by the sophisticated mechanism of autophagy and its crosstalk with Wnt signaling and other developmental pathways. Both autophagy and Wnt signaling are involved in embryogenesis and differentiation. Autophagy is responsible for degradation and recycling of cytosolic materials by directing them to lysosomes through the phagophore compartment. A dual feedback mechanism regulates the interface between autophagy and Wnt signaling pathways. During nutrient deprivation, beta-catenin and Dishevelled (essential Wnt signaling proteins) are targeted for autophagic degradation by LC3. When Wnt signaling is activated, beta-catenin acts as a corepressor of one of the autophagy proteins, p62. In contrast, another key Wnt signaling protein, GSK3 beta, negatively regulates the Wnt pathway and has been shown to induce autophagy by phosphorylation of the TSC complex. This article reviews the interplay between autophagy and Wnt signaling, describing how beta-catenin functions as a key cellular integration point coordinating proliferation with autophagy, and it discusses the clinical importance of the crosstalk between these mechanisms.
机译:细胞稳态和适应各种环境条件是由自噬和其串扰与WNT信号传导和其他发育途径的复杂机制来调节。自噬和WNT信号传导均涉及胚胎发生和分化。自噬负责通过将它们通过噬菌体隔室指导溶酶体来降解和再循环细胞溶质材料。双反馈机制调节自噬和WNT信令路径之间的界面。在营养剥夺期间,β-连环素和蓬蓬(必需的Wnt信号传导蛋白)靶向LC3的自噬降解。当激活WNT信号传导时,β-连环蛋白用作自噬蛋白,P62之一的核心压力。相反,另一个关键的Wnt信号蛋白GSK3β,负调节WNT途径,并且已被证明通过TSC复合物的磷酸化诱导自噬。本文审查了自噬和WNT信令之间的相互作用,描述了β-连环蛋白如何用作具有自噬的关键蜂窝积分点协调增殖的功能,并且探讨了这些机制之间串扰的临床重要性。

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