Chen Sung-Ho, Lin Jen-Kun, Liang Yu-Chih, Pan Min-Hsiung, Liu Shing-Hwa, Lin-Shiau Shoei-Yn
Institute of Toxicology, College of Medicine, National Taiwan University, Taipei, Taiwan.
Eur J Pharmacol. 2008 Oct 10;594(1-3):9-17. doi: 10.1016/j.ejphar.2008.07.024. Epub 2008 Jul 16.
Pyrrolidine dithiocarbamate (PDTC) is a metal chelator. Biologically, slight toxic affects EC50, 100+/-5.9 microM are observed when added to cultured HL-60 cells. CuCl2 at a physiological concentration (1 microM), but not FeCl2, Pb potentiated the cytotoxic effect of PDTC by 700 fold (EC50, 0.14+/-0.02 microM). Furthermore, results indicated that the PDTC/Cu complex induced an apoptotic process, evidenced by apoptotic bodies, DNA ladder and hypodiploidy cells. Additional studies showed that PDTC/Cu complex significantly decreased mitochondrial membrane potential, increased cytochrome c release, and reactive oxygen species production, and depleted reduced non-protein thiols in a time-dependent manner. Following oxidative stress, the PDTC/Cu complex sequentially activated JNK, NF-kappaB and AP-1 signaling pathways while IkappaB kinase activity was enhanced. The apoptotic process was eventually induced by caspase 3 activation and PARP degradation. The non-permeable copper-specific chelator-bathocuproine disulfonate (BCPS) and vitamin C were able to inhibit apoptosis and the elevation of intracellular Cu. Based on these findings; we conclude that PDTC/Cu complex-induced apoptosis is mediated by activation of JNK, NF-kappaB, AP-1 and caspase 3. Due to its high potency, PDTC may be useful as a therapeutic anti-cancer drug.
吡咯烷二硫代氨基甲酸盐(PDTC)是一种金属螯合剂。在生物学上,当将其添加到培养的HL-60细胞中时,会观察到轻微毒性,其半数有效浓度(EC50)为100±5.9微摩尔。生理浓度(1微摩尔)的氯化铜(CuCl2),而不是氯化亚铁(FeCl2)、铅,可使PDTC的细胞毒性作用增强700倍(EC50为0.14±0.02微摩尔)。此外,结果表明,PDTC/Cu复合物诱导了凋亡过程,凋亡小体、DNA梯带和亚二倍体细胞可证明这一点。进一步的研究表明,PDTC/Cu复合物可显著降低线粒体膜电位,增加细胞色素c释放、活性氧生成,并以时间依赖性方式消耗还原型非蛋白硫醇。氧化应激后,PDTC/Cu复合物依次激活JNK、NF-κB和AP-1信号通路,同时IκB激酶活性增强。凋亡过程最终由半胱天冬酶3激活和聚(ADP-核糖)聚合酶(PARP)降解诱导。不可渗透的铜特异性螯合剂—— bathocuproine disulfonate(BCPS)和维生素C能够抑制凋亡和细胞内铜的升高。基于这些发现,我们得出结论,PDTC/Cu复合物诱导的凋亡是由JNK、NF-κB、AP-1和半胱天冬酶3的激活介导的。由于其高效性,PDTC可能作为一种治疗性抗癌药物发挥作用。
