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HINT1在人肝癌细胞中抑制β-连环蛋白/TCF4、USF2和核因子κB的活性。

HINT1 inhibits beta-catenin/TCF4, USF2 and NFkappaB activity in human hepatoma cells.

作者信息

Wang Lin, Li Haiyang, Zhang Yujing, Santella Regina M, Weinstein I Bernard

机构信息

Department of Hepatobiliary Surgery, Kunming Medical College, Kunming, China.

出版信息

Int J Cancer. 2009 Apr 1;124(7):1526-34. doi: 10.1002/ijc.24072.

Abstract

In this study we explored the relevance of Hint, a novel tumor suppressor gene, to human hepatoma. The human hepatoma cell lines Hep3B and HepG2 express very low levels of the HINT1 protein but the Huh7 cells express a relatively high level. In Hep3B and HepG2 cells, but not in Huh7 cells, the promoter region of Hint1 is partially methylated and treatment with 5-azadcdeoxycytidine increased expression of the HINT1 protein and Hint1 mRNA in Hep3B and HepG2 cells. Increased expression of HINT1 in HepG2 cells markedly inhibited their growth. It also inhibited the transcriptional activities of beta-catenin/TCF4, and USF2, and inhibited the expression of endogenous cyclin D1 and TGFbeta2. Furthermore, HINT1 co-immunoprecipitated with USF2 in extracts of Hep2 cells. HINT1 also inhibited NFkappaB transcription factor reporter activity and inhibited translocation of the endogenous p65 protein to the nucleus of HepG2 cells. Therefore, decreased expression of the Hint1 gene through epigenetic silencing may play a role in enhancing the growth of a subset of human hepatoma by increasing the expression of genes controlled by the transcription factors beta-catenin, USF2, and NFkappaB.

摘要

在本研究中,我们探讨了一种新型肿瘤抑制基因Hint与人类肝癌的相关性。人类肝癌细胞系Hep3B和HepG2中HINT1蛋白表达水平极低,但Huh7细胞中表达水平相对较高。在Hep3B和HepG2细胞中,而非Huh7细胞中,Hint1的启动子区域部分甲基化,用5-氮杂-2'-脱氧胞苷处理可增加Hep3B和HepG2细胞中HINT1蛋白和Hint1 mRNA的表达。HepG2细胞中HINT1表达增加显著抑制其生长。它还抑制β-连环蛋白/TCF4和USF2的转录活性,并抑制内源性细胞周期蛋白D1和TGFβ2的表达。此外,HINT1在Hep2细胞提取物中与USF2共免疫沉淀。HINT1还抑制NFκB转录因子报告基因活性,并抑制内源性p65蛋白向HepG2细胞核的转运。因此,通过表观遗传沉默导致Hint1基因表达降低可能通过增加由转录因子β-连环蛋白、USF2和NFκB控制的基因表达,在促进一部分人类肝癌的生长中发挥作用。

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