组蛋白去乙酰化酶抑制剂与阿扎胞苷联合对食管癌细胞的选择性抑制作用
Selective inhibition of esophageal cancer cells by combination of HDAC inhibitors and Azacytidine.
作者信息
Ahrens Theresa D, Timme Sylvia, Hoeppner Jens, Ostendorp Jenny, Hembach Sina, Follo Marie, Hopt Ulrich T, Werner Martin, Busch Hauke, Boerries Melanie, Lassmann Silke
机构信息
a Dept. of Pathology; University Medical Center ; Freiburg , Germany.
出版信息
Epigenetics. 2015;10(5):431-45. doi: 10.1080/15592294.2015.1039216.
Esophageal cancers are highly aggressive tumors with poor prognosis despite some recent advances in surgical and radiochemotherapy treatment options. This study addressed the feasibility of drugs targeting epigenetic modifiers in esophageal squamous cell carcinoma (ESCC) and esophageal adenocarcinoma (EAC) cells. We tested inhibition of histone deacetylases (HDACs) by SAHA, MS-275, and FK228, inhibition of DNA methyltransferases by Azacytidine (AZA) and Decitabine (DAC), and the effect of combination treatment using both types of drugs. The drug targets, HDAC1/2/3 and DNMT1, were expressed in normal esophageal epithelium and tumor cells of ESCC or EAC tissue specimens, as well as in non-neoplastic esophageal epithelial (Het-1A), ESCC (OE21, Kyse-270, Kyse-410), and EAC (OE33, SK-GT-4) cell lines. In vitro, HDAC activity, histone acetylation, and p21 expression were similarly affected in non-neoplastic, ESCC, and EAC cell lines post inhibitor treatment. Combined MS-275/AZA treatment, however, selectively targeted esophageal cancer cell lines by inducing DNA damage, cell viability loss, and apoptosis, and by decreasing cell migration. Non-neoplastic Het-1A cells were protected against HDACi (MS-275)/AZA treatment. RNA transcriptome analyses post MS-275 and/or AZA treatment identified novel regulated candidate genes (up: BCL6, Hes2; down: FAIM, MLKL), which were specifically associated with the treatment responses of esophageal cancer cells. In summary, combined HDACi/AZA treatment is efficient and selective for the targeting of esophageal cancer cells, despite similar target expression of normal and esophageal cancer epithelium, in vitro and in human esophageal carcinomas. The precise mechanisms of action of treatment responses involve novel candidate genes regulated by HDACi/AZA in esophageal cancer cells. Together, targeting of epigenetic modifiers in esophageal cancers may represent a potential future therapeutic approach.
食管癌是侵袭性很强的肿瘤,尽管手术和放化疗治疗方案最近有所进展,但其预后仍然很差。本研究探讨了靶向表观遗传修饰剂的药物在食管鳞状细胞癌(ESCC)和食管腺癌(EAC)细胞中的可行性。我们测试了SAHA、MS-275和FK228对组蛋白去乙酰化酶(HDACs)的抑制作用,阿扎胞苷(AZA)和地西他滨(DAC)对DNA甲基转移酶的抑制作用,以及这两种药物联合治疗的效果。药物靶点HDAC1/2/3和DNMT1在正常食管上皮以及ESCC或EAC组织标本的肿瘤细胞中表达,也在非肿瘤性食管上皮(Het-1A)、ESCC(OE21、Kyse-270、Kyse-410)和EAC(OE33、SK-GT-4)细胞系中表达。在体外,抑制剂处理后,非肿瘤性、ESCC和EAC细胞系中的HDAC活性、组蛋白乙酰化和p21表达受到类似影响。然而,MS-275/AZA联合治疗通过诱导DNA损伤、细胞活力丧失和凋亡以及减少细胞迁移,选择性地靶向食管癌细胞系。非肿瘤性Het-1A细胞对HDACi(MS-275)/AZA治疗具有抗性。MS-275和/或AZA处理后的RNA转录组分析确定了新的调控候选基因(上调:BCL6、Hes2;下调:FAIM、MLKL),这些基因与食管癌细胞的治疗反应特异性相关。总之,尽管正常和食管癌上皮细胞中靶点表达相似,但HDACi/AZA联合治疗在体外和人食管癌中对靶向食管癌细胞是有效且有选择性的。治疗反应的确切作用机制涉及HDACi/AZA在食管癌细胞中调控的新候选基因。总之,靶向食管癌中的表观遗传修饰剂可能代表一种潜在的未来治疗方法。
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