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The postsynaptic density 95/disc-large/zona occludens protein syntenin directly interacts with Frizzled 7 and supports noncanonical Wnt signaling

机译:突触后密度95 /盘大/区域闭合蛋白合成蛋白与卷曲蛋白7直接相互作用并支持非经典Wnt信号传导

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摘要

Wnt signaling pathways are essential for embryonic patterning, and they are disturbed in a wide spectrum of diseases, including cancer. An unresolved question is how the different Wnt pathways are supported and regulated. We previously established that the postsynaptic density 95/disc-large/zona occludens (PDZ) protein syntenin binds to syndecans, Wnt coreceptors, and known stimulators of protein kinase C (PKC)alpha and CDC42 activity. Here, we show that syntenin also interacts with the C-terminal PDZ binding motif of several Frizzled Wnt receptors, without compromising the recruitment of Dishevelled, a key downstream Wnt-signaling component. Syntenin is coexpressed with cognate Frizzled during early development in Xenopus. Overexpression and down-regulation of syntenin disrupt convergent extension movements, supporting a role for syntenin in noncanonical Wnt signaling. Syntenin stimulates c-jun phosphorylation and modulates Frizzled 7 signaling, in particular the PKC alpha/CDC42 noncanonical Wnt signaling cascade. The syntenin-Frizzled 7 binding mode indicates syntenin can accommodate Frizzled 7-syndecan complexes. We propose that syntenin is a novel component of the Wnt signal transduction cascade and that it might function as a direct intracellular link between Frizzled and syndecans.
机译:Wnt信号通路对于胚胎的形成至关重要,在包括癌症在内的各种疾病中都受到干扰。一个尚未解决的问题是如何支持和调节不同的Wnt途径。我们先前建立的突触后密度95 /盘大/分区闭塞(PDZ)蛋白syntenin绑定到syndecans,Wnt核心受体和已知的蛋白激酶C(PKC)alpha和CDC42活性刺激物。在这里,我们显示syntenin还可与数个卷曲的Wnt受体的C末端PDZ结合基序相互作用,而不会损害Dishevelled(关键的下游Wnt信号传导成分)的募集。 Syntenin在非洲爪蟾的早期发育过程中与同源的Frizzled共表达。 Syntenin的过表达和下调破坏了聚合延伸运动,支持了syntenin在非经典Wnt信号传导中的作用。 Syntenin刺激c-jun磷酸化并调节Frizzled 7信号传导,特别是PKC alpha / CDC42非规范Wnt信号传导级联。 syntenin-Frizzled 7结合模式表明syntenin可以容纳Frizzled 7-syndecan复合物。我们建议syntenin是Wnt信号转导级联的一个新颖的组成部分,并且它可能充当Frizzled和syndecans之间的直接细胞内链接。

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