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人鲟鱼钙蛋白-1与细胞核和细胞质蛋白相互作用,并作为一种小泛素样修饰物E3连接酶发挥作用。

Human stanniocalcin-1 interacts with nuclear and cytoplasmic proteins and acts as a SUMO E3 ligase.

作者信息

dos Santos Marcos Tadeu, Trindade Daniel Maragno, Gonçalves Kaliandra de Almeida, Bressan Gustavo Costa, Anastassopoulos Filipe, Yunes José Andres, Kobarg Jörg

机构信息

Laboratório Nacional de Biociências, Centro Nacional de Pesquisa em Energia e Materiais, Rua Giuseppe Máximo Scolfaro 10.000, CP6192, 13084-971 Campinas, SP, Brasil.

出版信息

Mol Biosyst. 2011 Jan;7(1):180-93. doi: 10.1039/c0mb00088d. Epub 2010 Nov 1.

DOI:10.1039/c0mb00088d
PMID:21042649
Abstract

Human stanniocalcin-1 (STC1) is a glycoprotein that has been implicated in different physiological process, including angiogenesis, apoptosis and carcinogenesis. Here we identified STC1 as a putative molecular marker for the leukemic bone marrow microenvironment and identified new interacting protein partners for STC1. Seven selected interactions retrieved from yeast two-hybrid screens were confirmed by GST-pull down assays in vitro. The N-terminal region was mapped to be the region that mediates the interaction with cytoplasmic, mitochondrial and nuclear proteins. STC1 interacts with SUMO-1 and several proteins that have been shown to be SUMOylated and localized to SUMOylation related nuclear bodies. Although STC1 interacts with SUMO-1 and has a high theoretical prediction score for a SUMOylation site, endogenous co-immunoprecipitation and in vitro SUMOylation assays with the purified recombinant protein could not detect STC1 SUMOylation. However, when we tested STC1 for SUMO E3 ligase activity, we found in an in vitro assay, that it significantly increases the SUMOylation of two other proteins. Confocal microscopic subcellular localization studies using both transfected cells and specific antibodies for endogenous STC1 revealed a cytoplasmic and nuclear deposition, the latter in the form of some specific dot-like substructure resembling SUMOylation related nuclear bodies. Together, these findings suggest a new role for STC1 in SUMOylation pathways, in nuclear bodies.

摘要

人鲽源钙调蛋白-1(STC1)是一种糖蛋白,参与了包括血管生成、细胞凋亡和致癌作用在内的多种生理过程。在此,我们将STC1鉴定为白血病骨髓微环境的一种假定分子标志物,并确定了STC1新的相互作用蛋白伙伴。通过体外GST下拉实验证实了从酵母双杂交筛选中获得的7种选定的相互作用。N端区域被定位为介导与细胞质、线粒体和核蛋白相互作用的区域。STC1与SUMO-1以及几种已被证明发生SUMO化并定位于SUMO化相关核体的蛋白相互作用。尽管STC1与SUMO-1相互作用且对SUMO化位点有较高的理论预测得分,但内源性免疫共沉淀和用纯化重组蛋白进行的体外SUMO化实验均未检测到STC1的SUMO化。然而,当我们检测STC1的SUMO E3连接酶活性时,我们在体外实验中发现,它能显著增加另外两种蛋白的SUMO化。使用转染细胞和针对内源性STC1的特异性抗体进行的共聚焦显微镜亚细胞定位研究显示,STC1在细胞质和细胞核中均有沉积,后者以一些类似SUMO化相关核体的特定点状亚结构的形式存在。总之,这些发现提示STC1在核体中的SUMO化途径中具有新的作用。

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