首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Identification of a Structural Motif in the Tumor-Suppressive Protein GRIM-19 Required for Its Antitumor Activity
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Identification of a Structural Motif in the Tumor-Suppressive Protein GRIM-19 Required for Its Antitumor Activity

机译:肿瘤抑制蛋白GRIM-19中其抗肿瘤活性所需的结构基元的鉴定

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摘要

We have previously isolated GRIM-19, a novel growth suppressor, using a genetic method. GRIM-19 ablates cell growth by inhibiting the transcription factor signal transducer and activator of transcription 3 (STAT3). Up-regulation of STAT3 and growth promotion were observed in a number of human tumors. Although the tumor-suppressive actions of GRIM-19 are known, the structural elements required for its antitumor actions are not understood. Mutational and protein sequence analyses identified a motif in the N terminus of GRIM-19 that exhibited similarity to certain RNA viral proteins. We show that disruption of specific amino acids within this motif cripples the antitumor actions of GRIM-19. These mutants fail to interact with STAT3 efficiently and consequently do not inhibit growth-promoting gene expression. More importantly, we show that a clinically observed mutation in the N terminus of GRIM-19 also weakened its interaction with STAT3 and antitumor action. Together, these studies identify a major role for the N terminus of GRIM-19 in mediating its tumor-suppressive actions.
机译:我们以前已经使用遗传方法分离出了新型生长抑制剂GRIM-19。 GRIM-19通过抑制转录因子信号转导子和转录激活子3(STAT3)消除细胞生长。在许多人类肿瘤中观察到STAT3的上调和生长促进。尽管已知GRIM-19的肿瘤抑制作用,但其抗肿瘤作用所需的结构元件尚不清楚。突变和蛋白质序列分析确定了GRIM-19 N末端的一个基序,该基序与某些RNA病毒蛋白具有相似性。我们显示该主题内特定氨基酸的破坏削弱了GRIM-19的抗肿瘤作用。这些突变体不能有效地与STAT3相互作用,因此不抑制促进生长的基因表达。更重要的是,我们显示临床观察到的GRIM-19 N端突变也减弱了它与STAT3的相互作用和抗肿瘤作用。总之,这些研究确定了GRIM-19 N末端在介导其肿瘤抑制作用中的主要作用。

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