海洋三萜糖苷 frondoside A 诱导尿路上皮癌细胞发生 p53 非依赖性细胞凋亡并抑制自噬。
The marine triterpene glycoside frondoside A induces p53-independent apoptosis and inhibits autophagy in urothelial carcinoma cells.
机构信息
Laboratory of Experimental Oncology, Department of Oncology, Hematology and Bone Marrow Transplantation with Section Pneumology, University Medical Center Hamburg-Eppendorf, Martinistr. 52, Hamburg, 20246, Germany.
Laboratory of Marine Natural Products Chemistry, G.B. Elyakov Pacific Institute of Bioorganic Chemistry, Far-East Branch, Russian Academy of Sciences, Prospekt 100-let Vladivostoku 159, Vladivostok, 690022, Russian Federation.
出版信息
BMC Cancer. 2017 Feb 1;17(1):93. doi: 10.1186/s12885-017-3085-z.
BACKGROUND
Advanced urothelial carcinomas represent a considerable clinical challenge as they are difficult to treat. Platinum-based combination regimens obtain response rates ranging from 40 to 70% in first-line therapy of advanced urothelial carcinoma. In the majority of cases, however, the duration of these responses is limited, and when progression occurs, the outcome is generally poor. Therefore, novel therapeutic strategies are urgently needed. The purpose of the current research is to investigate the anticancer effects and the mode of action of the marine triterpene glycoside frondoside A in p53-wild type and p53-deficient human urothelial carcinoma cells.
METHODS
Activity of frondoside A was examined in the human urothelial carcinoma cell lines RT112, RT4, HT-1197, TCC-SUP, T-24, and 486p. Effects of frondoside A on cell viability, either alone or in combination with standard cytotoxic agents were investigated, and synergistic effects were analyzed. Pro-apoptotic activity was assessed by Western blotting and FACS, alone and in combination with a caspases-inhibitor. The impact of functional p53 was investigated by siRNA gene silencing and the p53 inhibitor pifithrin-α. Effects on autophagy were studied using LC3B-I/II and SQSTM/p62 as markers. The unpaired Student's t-test was used for comparison of the data sets.
RESULTS
Frondoside A shows high cytotoxicity in urothelial carcinoma cells with IC ranging from 0.55 to 2.33 μM while higher concentrations of cisplatin are required for comparable effects (IC = 2.03 ~ 5.88 μM). Induction of apoptosis by frondoside A was associated with the regulation of several pro-apoptotic factors, like caspase-3, -8, and -9, PARP, Bax, p21, DNA fragmentation, and externalization of phosphatidylserine. Remarkably, inhibition of p53 by gene silencing or pifithrin-α pretreatment, as well as caspase inhibition, did not suppress apoptotic activity of frondoside A, while cisplatin activity, in contrast, was significantly decreased. Frondoside A inhibited pro-survival autophagy, a known mechanism of drug resistance in urothelial carcinoma and showed synergistic activity with cisplatin and gemcitabine.
CONCLUSIONS
A unique combination of properties makes marine compound frondoside A a promising candidate for the treatment of human urothelial carcinomas.
背景
高级尿路上皮癌是一个相当大的临床挑战,因为它们很难治疗。在一线治疗高级尿路上皮癌中,基于铂的联合方案的反应率在 40%至 70%之间。然而,在大多数情况下,这些反应的持续时间有限,当进展发生时,结果通常较差。因此,迫切需要新的治疗策略。本研究的目的是研究海洋三萜糖苷佛司可林 A 在 p53 野生型和 p53 缺失型人尿路上皮癌细胞中的抗癌作用和作用机制。
方法
在人尿路上皮癌细胞系 RT112、RT4、HT-1197、TCC-SUP、T-24 和 486p 中检测佛司可林 A 的活性。单独或与标准细胞毒性药物联合检测佛司可林 A 对细胞活力的影响,并分析协同作用。通过 Western blot 和 FACS 单独和与半胱天冬酶抑制剂联合评估促凋亡活性。通过 siRNA 基因沉默和 p53 抑制剂 pifithrin-α 研究功能 p53 的影响。使用 LC3B-I/II 和 SQSTM/p62 作为标记物研究自噬的影响。使用未配对的学生 t 检验比较数据集。
结果
佛司可林 A 在尿路上皮癌细胞中具有高细胞毒性,IC 范围为 0.55 至 2.33 μM,而需要更高浓度的顺铂才能达到类似的效果(IC = 2.03 至 5.88 μM)。佛司可林 A 诱导的细胞凋亡与几种促凋亡因子的调节有关,如 caspase-3、-8 和 -9、PARP、Bax、p21、DNA 片段化和磷脂酰丝氨酸的外化。值得注意的是,基因沉默或 pifithrin-α 预处理抑制 p53 以及 caspase 抑制均不能抑制佛司可林 A 的凋亡活性,而顺铂活性则显著降低。佛司可林 A 抑制了生存相关的自噬,这是尿路上皮癌中一种已知的耐药机制,并与顺铂和吉西他滨表现出协同作用。
结论
海洋化合物佛司可林 A 具有独特的特性组合,使其成为治疗人类尿路上皮癌的有前途的候选药物。
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