通过计算机和实验分析预测EZH2抑制剂GSK343通过诱导金属硫蛋白基因对肝细胞癌的治疗价值

Tsang‐Pai Liu, Yi-Han Hong, K. Tung, Pei-Ming Yang
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引用次数: 18

摘要

肝细胞癌(HCC)是全球第三大癌症相关死亡原因,目前尚无有效的分子靶向治疗方法。zeste homolog 2的增强子(Enhancer of zeste homolog 2, EZH2)是一种组蛋白H3赖氨酸27 (H3K27)特异性甲基转移酶,已成为新的抗癌靶点。我们之前的研究表明,EZH2的s -腺苷- l-甲硫氨酸(SAM)竞争性抑制剂GSK343在包括HCC在内的癌细胞中诱导自噬并增强药物敏感性。本研究通过计算机研究发现,EZH2在HCC患者癌组织中均在基因和蛋白水平上过表达。微阵列分析和体外实验表明,GSK343的抗hcc活性与金属硫蛋白(MT)基因的诱导有关。此外,在公共基因表达数据库中发现EZH2和MT1/MT2A基因在癌细胞系和组织中呈负相关。综上所述,我们的研究结果表明EZH2抑制剂可能是HCC的良好治疗选择,并且诱导MT基因与EZH2抑制剂的抗HCC活性相关。
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In silico and experimental analyses predict the therapeutic value of an EZH2 inhibitor GSK343 against hepatocellular carcinoma through the induction of metallothionein genes
There are currently no effective molecular targeted therapies for hepatocellular carcinoma (HCC), the third leading cause of cancer-related death worldwide. Enhancer of zeste homolog 2 (EZH2), a histone H3 lysine 27 (H3K27)-specific methyltransferase, has been emerged as novel anticancer target. Our previous study has demonstrated that GSK343, an S-adenosyl-L-methionine (SAM)-competitive inhibitor of EZH2, induces autophagy and enhances drug sensitivity in cancer cells including HCC. In this study, an in silico study was performed and found that EZH2 was overexpressed in cancerous tissues of HCC patients at both gene and protein levels. Microarray analysis and in vitro experiments indicated that the anti-HCC activity of GSK343 was associated with the induction of metallothionein (MT) genes. In addition, the negative association of EZH2 and MT1/MT2A genes in cancer cell lines and tissues was found in public gene expression database. Taken together, our findings suggest that EZH2 inhibitors could be a good therapeutic option for HCC, and induction of MT genes was associated with the anti-HCC activity of EZH2 inhibitors.
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