EZH2 inhibition re-sensitizes multidrug resistant B-cell lymphomas to etoposide mediated apoptosis

M. Smonskey, E. Lasorsa, S. Rosario, J. Kirk, F. Hernandez-Ilizaliturri, L. Ellis
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引用次数: 12

Abstract

Reactivation of apoptotic pathways is an attractive strategy for patients with treatment-resistant B-cell lymphoma. The tumor suppressor, p53 is central for apoptotic response to multiple DNA damaging agents used to treat aggressive B-cell lymphomas, including etoposide. It has been demonstrated that etoposide induced DNA damage and therapeutic efficacy is enhanced by combination with inhibitors of the histone methyltransferase, enhancer of zeste homolog 2 (EZH2). Further, EZH2 was identified to regulate cell fate decisions in response to DNA damage. Using B-cell lymphoma cell lines resistant to etoposide induced cell death; we show that p53 is dramatically down regulated and MDMX, a negative regulator of p53, is significantly up regulated. However, these cell lines remain responsive to etoposide mediated DNA damage and exhibit cell cycle inhibition and induction of senescence. Furthermore, chemical inhibition of EZH2 directs DNA damage to a predominant p53 dependent apoptotic response associated with loss of MDMX and BCL-XL. These data provide confirmation of EZH2 in determining cell fate following DNA damage and propose a novel therapeutic strategy for patients with aggressive treatment-resistant B-cell lymphoma.
EZH2抑制使多药耐药b细胞淋巴瘤对依托泊苷介导的凋亡再敏感
凋亡通路的再激活是治疗抵抗性b细胞淋巴瘤患者的一个有吸引力的策略。肿瘤抑制因子p53是用于治疗侵袭性b细胞淋巴瘤的多种DNA损伤剂(包括依托泊苷)的凋亡反应的核心。研究表明,依托波苷与组蛋白甲基转移酶抑制剂、zeste同源物2的增强剂(enhancer of zeste homolog 2, EZH2)联合使用可增强其诱导的DNA损伤和治疗效果。此外,EZH2被鉴定为在DNA损伤响应中调节细胞命运决定。对依托泊苷耐药的b细胞淋巴瘤细胞系诱导细胞死亡我们发现p53被显著下调,而p53的负调节因子MDMX被显著上调。然而,这些细胞系仍然对依托泊苷介导的DNA损伤有反应,并表现出细胞周期抑制和诱导衰老。此外,EZH2的化学抑制将DNA损伤导向与MDMX和BCL-XL缺失相关的主要p53依赖性凋亡反应。这些数据证实了EZH2在DNA损伤后决定细胞命运的作用,并为侵袭性治疗抵抗性b细胞淋巴瘤患者提供了一种新的治疗策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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