TRIM67 蛋白通过降解 80K-H 负调控 Ras 活性并诱导神经突生成。
TRIM67 protein negatively regulates Ras activity through degradation of 80K-H and induces neuritogenesis.
机构信息
Department of Biochemistry, Hokkaido University Graduate School of Medicine, Sapporo, Hokkaido 060-8638, Japan.
出版信息
J Biol Chem. 2012 Apr 6;287(15):12050-9. doi: 10.1074/jbc.M111.307678. Epub 2012 Feb 15.
Abstract
Tripartite motif (TRIM)-containing proteins, which are defined by the presence of a common domain structure composed of a RING finger, one or two B-box motifs and a coiled-coil motif, are involved in many biological processes including innate immunity, viral infection, carcinogenesis, and development. Here we show that TRIM67, which has a TRIM motif, an FN3 domain and a SPRY domain, is highly expressed in the cerebellum and that TRIM67 interacts with PRG-1 and 80K-H, which is involved in the Ras-mediated signaling pathway. Ectopic expression of TRIM67 results in degradation of endogenous 80K-H and attenuation of cell proliferation and enhances neuritogenesis in the neuroblastoma cell line N1E-115. Furthermore, morphological and biological changes caused by knockdown of 80K-H are similar to those observed by overexpression of TRIM67. These findings suggest that TRIM67 regulates Ras signaling via degradation of 80K-H, leading to neural differentiation including neuritogenesis.
摘要
三基序(TRIM)蛋白包含蛋白,其特征在于存在由一个 RING 指、一个或两个 B-box 基序和一个卷曲螺旋基序组成的共同结构域,参与许多生物学过程,包括先天免疫、病毒感染、致癌作用和发育。在这里,我们显示具有 TRIM 基序、FN3 结构域和 SPRY 结构域的 TRIM67 在小脑中有高表达,并且 TRIM67 与 PRG-1 和 80K-H 相互作用,后者涉及 Ras 介导的信号通路。TRIM67 的异位表达导致内源性 80K-H 的降解,从而减弱细胞增殖并增强神经母细胞瘤细胞系 N1E-115 中的神经突生成。此外,由 80K-H 敲低引起的形态和生物学变化与观察到的 TRIM67 过表达相似。这些发现表明,TRIM67 通过降解 80K-H 来调节 Ras 信号,从而导致包括神经突生成在内的神经分化。
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