Department of Biochemistry, National Defense Medical Center, Taipei 114, Taiwan, ROC.
Int J Biochem Cell Biol. 2011 Dec;43(12):1720-8. doi: 10.1016/j.biocel.2011.08.006. Epub 2011 Aug 12.
The anthracyclin antibiotic agent doxorubicin (DXR) has been widely used as a chemotherapeutic drug for more than 40 years, but its clinical use has been limited by its cardiotoxicity. The mechanism of action of DXR remains uncertain and controversial. A series of 1,2-heteroannelated anthraquinones and anthra[1,2-d]imidazole-6,11-dione compounds were synthesized and their cytotoxicity profiles were analyzed using the National Cancer Institute 60 (NCI 60) platform and human telomerase inhibition assays. In the current study, three of the 1,2-heteroannelated anthraquinones, NSC745795, NSC745885 and NSC745887, were found to differ from each other with respect to their effects on cell cycle regulation, apoptosis, autophagy, senescence and their abilities to induce DNA damage. The differences depended on the presence or absence of a heterocyclic moiety, which suggested that the differences were due, at least in part, to differential effects on specific cellular targets, such as p53. In contrast to DXR, which induced p53 expression, treatment with NSC745885 resulted in the degradation of several proteins, including p53, via proteasome-dependent and -independent pathways in HeLa cells. These results provide insights into the molecular mechanisms governing cell inhibition by 1,2-heteroannelated anthraquinone derivatives and suggest that these mechanisms could serve as the basis for new structure-based drug designs.
蒽环类抗生素阿霉素(DXR)已广泛用作化疗药物超过 40 年,但由于其心脏毒性,其临床应用受到限制。DXR 的作用机制仍不确定且存在争议。合成了一系列 1,2-杂芳基蒽醌和蒽[1,2-d]咪唑-6,11-二酮化合物,并使用国家癌症研究所 60(NCI 60)平台和人端粒酶抑制测定法分析了它们的细胞毒性特征。在本研究中,三种 1,2-杂芳基蒽醌,NSC745795、NSC745885 和 NSC745887,在调节细胞周期、凋亡、自噬、衰老和诱导 DNA 损伤的能力方面表现出不同的作用。这些差异取决于杂环部分的存在与否,这表明差异至少部分归因于对特定细胞靶标的差异作用,例如 p53。与诱导 p53 表达的 DXR 不同,用 NSC745885 处理会导致 HeLa 细胞中 p53 等几种蛋白质通过蛋白酶体依赖性和非依赖性途径降解。这些结果深入了解了 1,2-杂芳基蒽醌衍生物抑制细胞的分子机制,并表明这些机制可以作为新的基于结构的药物设计的基础。
