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蛋白磷酸酶1H在结肠腺癌中过表达,与CSE1L相关。

Protein phosphatase 1H, overexpressed in colon adenocarcinoma, is associated with CSE1L.

作者信息

Sugiura Takeyuki, Noguchi Yoshie, Sakurai Kayo, Hattori Chiharu

机构信息

Discovery Research Laboratory, Tokyo R&D Center, Daiichi Pharmaceutical Co. Ltd., Daiichi-Sankyo Group, Tokyo, Japan.

出版信息

Cancer Biol Ther. 2008 Feb;7(2):285-92. doi: 10.4161/cbt.7.2.5302. Epub 2007 Nov 14.

DOI:10.4161/cbt.7.2.5302
PMID:18059182
Abstract

In search for a new anticancer drug target, we explored genes involved in colon adenocarcinoma development through dysregulation of a signal transduction pathway. By using the gene expression profile database, we found protein phosphatase 1H (PPM1H), belonging to the protein phosphatase 2C (PP2C) family, upregulated in colon adenocarcinomas compared with normal colon tissues. RT-PCR analysis verified the elevated level of PPM1H expression in colon cancer cell lines relative to a normal colon cell line. PPM1H encodes a protein with a molecular mass of approximately 50 kDa that resides in the cytoplasm. PPM1H fused with maltose-binding protein expressed in E. coli exhibited phosphatase activity characteristic of the PP2C family. Co-immunoprecipitation coupled with mass spectrometry analysis identified CSE1L, a proliferation and apoptosis-related protein, as a PPM1H-interacting protein. Native, but not inactive, PPM1H expressed in HeLa cells increased the mobility of CSE1L on SDS gels and a similar mobility shift was observed for purified CSE1L after treatment with PPM1H in vitro, supporting the notion that CSE1L is a substrate of PPM1H. Dominant negative PPM1H protected HeLa cells from cell death triggered by staurosporine or taxol. Additionally, knockdown of PPM1H expression with small interfering RNAs suppressed the growth of MCF-7 cells weakly but consistently. PPM1H controls cell cycle and proliferation of cancer cells potentially through dephosphorylation of CSE1L and might be a new target of anticancer drugs.

摘要

为寻找新的抗癌药物靶点,我们通过信号转导通路的失调来探索参与结肠腺癌发生发展的基因。利用基因表达谱数据库,我们发现属于蛋白磷酸酶2C(PP2C)家族的蛋白磷酸酶1H(PPM1H)在结肠腺癌中相对于正常结肠组织上调。RT-PCR分析证实结肠癌细胞系中PPM1H的表达水平相对于正常结肠细胞系有所升高。PPM1H编码一种分子量约为50 kDa的蛋白,定位于细胞质中。与在大肠杆菌中表达的麦芽糖结合蛋白融合的PPM1H表现出PP2C家族特有的磷酸酶活性。免疫共沉淀结合质谱分析鉴定出增殖和凋亡相关蛋白CSE1L为与PPM1H相互作用的蛋白。在HeLa细胞中表达的天然而非无活性的PPM1H增加了CSE1L在SDS凝胶上的迁移率,并且在用PPM1H体外处理纯化的CSE1L后也观察到了类似的迁移率变化,这支持了CSE1L是PPM1H底物的观点。显性负性PPM1H保护HeLa细胞免受星形孢菌素或紫杉醇引发的细胞死亡。此外,用小干扰RNA敲低PPM1H的表达可微弱但持续地抑制MCF-7细胞的生长。PPM1H可能通过使CSE1L去磷酸化来控制癌细胞的细胞周期和增殖,可能是抗癌药物的新靶点。

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