State Key Laboratory of Natural Medicines, China Pharmaceutical University, Nanjing 210009, PR China.
J Med Chem. 2013 Jun 13;56(11):4641-55. doi: 10.1021/jm400393u. Epub 2013 May 16.
A series of hybrids from O(2)-(2,4-dinitrophenyl)diazeniumdiolate and oleanolic acid (OA) were designed, synthesized, and biologically evaluated as novel nitric oxide (NO)-releasing prodrugs that could be activated by glutathione S-transferase π (GSTπ) overexpressed in a number of cancer cells. It was discovered that the most active compound, 21, released high levels of NO selectively in HCC cells but not in the normal cells and exhibited potent antiproliferative activity in vitro as well as remarkable tumor-retarding effects in vivo. Compared with the reported GSTπ-activated prodrugs JS-K and PABA/NO, 21 exhibited remarkably improved stability in the absence of GSTπ. Importantly, the decomposition of 21 occurred in the presence of GSTπ and was much more effective than in glutathione S-transferase α. Additionally, 21 induced apoptosis in HepG2 cells by arresting the cell cycle at the G2/M phase, activating both the mitochondrion-mediated pathway and the MAPK pathway and enhancing the intracellular production of ROS.
设计、合成并生物评价了一系列 O(2)-(2,4-二硝基苯基)重氮二氢氧化物和齐墩果酸 (OA) 的杂合化合物,作为新型一氧化氮 (NO) 释放前药,可被多种癌细胞中过表达的谷胱甘肽 S-转移酶 π (GSTπ) 激活。结果发现,最活跃的化合物 21 能选择性地在 HCC 细胞中释放高水平的 NO,而在正常细胞中则不会,并且在体外表现出很强的抗增殖活性,在体内也有显著的肿瘤抑制作用。与已报道的 GSTπ 激活前药 JS-K 和 PABA/NO 相比,21 在没有 GSTπ 的情况下表现出显著提高的稳定性。重要的是,21 的分解在 GSTπ 存在的情况下发生,而且比在谷胱甘肽 S-转移酶 α 中更有效。此外,21 通过将细胞周期阻滞在 G2/M 期,激活线粒体介导的途径和 MAPK 途径,增强细胞内 ROS 的产生,诱导 HepG2 细胞凋亡。
