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豆蔻酰化裸 2 通过降解质膜上的 Dishevelled-1 拮抗 Wnt-β-连环蛋白活性。

Myristoylated Naked2 antagonizes Wnt-beta-catenin activity by degrading Dishevelled-1 at the plasma membrane.

机构信息

Cancer Research Center, Xiamen University Medical College, Xiamen, 361005 Fujian, China.

出版信息

J Biol Chem. 2010 Apr 30;285(18):13561-8. doi: 10.1074/jbc.M109.075945. Epub 2010 Feb 20.

Abstract

In Drosophila, naked cuticle is an inducible antagonist of the Wnt-beta-catenin pathway, likely acting at the level of Dishevelled (Dsh/Dvl), an essential component of this pathway. The mechanism by which naked cuticle and its two vertebrate orthologs, Naked1 (NKD1) and Naked2 (NKD2), inhibit Dvl function is unknown. NKD2 is myristoylated, a co-translational modification that leads to its plasma membrane localization. In contrast, myristoylation-deficient G2A NKD2 is cytoplasmic. Herein we show that the ability of Nkd2/NKD2 to antagonize Wnt-beta-catenin activity during zebrafish embryonic development and in mammalian HEK293 cells is myristoylation-dependent. NKD2 and Dvl-1 interact and co-localize at the lateral membrane of polarized epithelial cells. In reciprocal overexpression and siRNA knockdown experiments, NKD2 and Dvl-1 destabilize each other via enhanced polyubiquitylation; this effect is also dependent upon Naked2 myristoylation. Cell fractionation and ubiquitylation assays indicate that endogenous NKD2 interacts with a slower migrating, ubiquitylated form of Dvl-1 in plasma membrane fractions. These results provide a mechanism by which NKD2 antagonizes Wnt signaling: myristoylated NKD2 interacts with Dvl-1 at the plasma membrane, and this interaction leads to their mutual ubiquitin-mediated proteasomal degradation.

摘要

在果蝇中,裸皮是 Wnt-β-连环蛋白途径的诱导性拮抗剂,可能作用于该途径的必需组成部分 Dishevelled(Dsh/Dvl)。裸皮及其两种脊椎动物同源物 Naked1(NKD1)和 Naked2(NKD2)抑制 Dvl 功能的机制尚不清楚。NKD2 是豆蔻酰化的,这是一种翻译后修饰,导致其定位于质膜。相比之下,缺乏豆蔻酰化的 G2A NKD2 是细胞质的。本文表明,Nkd2/NKD2 在斑马鱼胚胎发育和哺乳动物 HEK293 细胞中拮抗 Wnt-β-连环蛋白活性的能力依赖于豆蔻酰化。NKD2 和 Dvl-1 在极化上皮细胞的侧膜相互作用并共定位。在相互过表达和 siRNA 敲低实验中,NKD2 和 Dvl-1 通过增强多泛素化相互破坏彼此;这种效应也依赖于 Naked2 的豆蔻酰化。细胞分级分离和泛素化测定表明,内源性 NKD2 与质膜部分中迁移速度较慢、泛素化的 Dvl-1 相互作用。这些结果提供了 Naked2 拮抗 Wnt 信号的机制:豆蔻酰化的 Naked2 与质膜上的 Dvl-1 相互作用,这种相互作用导致它们相互的泛素介导的蛋白酶体降解。

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