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Rnf25/AO7通过破坏Nkd1-Axin抑制复合物来正向调节Wnt信号通路,且不依赖于其泛素连接酶活性。

Rnf25/AO7 positively regulates wnt signaling via disrupting Nkd1-Axin inhibitory complex independent of its ubiquitin ligase activity.

作者信息

Gao Rui, Ma Lin-Qiang, Du Xiaogang, Zhang Ting-Ting, Zhao Liang, Liu Luhong, Liu Jing-Crystal, Guo Fengjin, Cheng Zhi, Huang Huizhe

机构信息

Second Affiliated Hospital, Chongqing Medical University, Chongqing, China 400010.

出版信息

Oncotarget. 2016 Apr 26;7(17):23850-9. doi: 10.18632/oncotarget.8126.

Abstract

Wnt signaling components have been shown to control key events in embryogenesis and to maintain tissue homeostasis in the adult. Nkd1/2 and Axin1/2 protein families are required for feedback regulation of Wnt signaling. The mechanisms by which Nkd1 and Nkd2 exhibit significant differences in signal transduction remain incompletely understood. Here we report that Rnf25/AO7, a previously identified E3 ubiquitin ligase for Nkd2, physically interacts with Nkd1 and Axin in an E3 ligase-independent manner to strengthen Wnt signalling. To determine the biological role of Rnf25 in vivo, we found that the renal mesenchymal cell, in which rnf25 was knocked-down, also exhibited more epithelial characters than MOCK control. Meanwhile, the transcriptional level of rnf25 was elevated in three separate tumor tissues more than that in paracarcinomatous tissue. Depletion of Rnf25 in zebrafish embryos attenuated transcriptions of maternal and zygotic Wnt target genes. Our results indicated that Rnf25 might serve as a molecular device, controlling the different antagonizing functions against canonical Wnt signaling between Nkd1 and Nkd2 cooperated with Axin.

摘要

Wnt信号通路的组成部分已被证明可控制胚胎发育中的关键事件,并维持成体组织的稳态。Nkd1/2和Axin1/2蛋白家族是Wnt信号通路反馈调节所必需的。Nkd1和Nkd2在信号转导中表现出显著差异的机制仍未完全了解。在此,我们报告Rnf25/AO7,一种先前鉴定的Nkd2的E3泛素连接酶,以一种不依赖E3连接酶的方式与Nkd1和Axin发生物理相互作用,从而增强Wnt信号。为了确定Rnf25在体内的生物学作用,我们发现敲低rnf25的肾间充质细胞比MOCK对照表现出更多的上皮特征。同时,在三个独立的肿瘤组织中,rnf25的转录水平比癌旁组织中的转录水平升高。斑马鱼胚胎中Rnf25的缺失减弱了母源和合子Wnt靶基因的转录。我们的结果表明,Rnf25可能作为一种分子装置,与Axin协同控制Nkd1和Nkd2对经典Wnt信号的不同拮抗功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a42d/5029668/d661e5f9a944/oncotarget-07-23850-g001.jpg

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