Department of Chemical Sciences, University of Naples Federico II, Complesso Universitario di Monte Sant'Angelo, via Cinthia 21, 80126, Naples, Italy.
EMBL, CS 90181, 71 AV des Martyrs, 38009, Grenoble (38), France.
ChemMedChem. 2019 Mar 5;14(5):594-602. doi: 10.1002/cmdc.201800805. Epub 2019 Feb 11.
The effects of encapsulating the cytotoxic dinuclear trithiolato-bridged arene ruthenium complex [(η -p-MeC H iPr) Ru (μ -S-p-C H tBu) ]Cl (DiRu-1) within the apoferritin (AFt) nanocage were investigated. The DiRu-1-AFt nanocarrier was characterized by UV/Vis spectroscopy, ICP-MS, CD and X-ray crystallography. In contrast to previously reported Au- and Pt-based drug-loaded AFt carriers, we found no evidence of direct interactions between DiRu-1 and AFt. DiRu-1-AFt is cytotoxic toward immortalized murine BALB/c-3T3 fibroblasts transformed with SV40 virus (SVT2) and human epidermoid carcinoma A431 malignant cells, and exhibits moderate selectivity for these cancer cells over normal BALB/c-3T3 cells. DiRu-1-AFt triggers the production of reactive oxygen species, depolarization of mitochondrial membrane potential, and induces cell death via p53-mediated apoptosis. Comparison between our data and previous results suggests that the presence of specific interactions between a metal-based drug and AFt within the protein cage is not essential for drug encapsulation.
将细胞毒性双核三硫代桥联芳烃钌配合物[(η-p-MeC H iPr)Ru(μ-S-p-C H tBu)]Cl(DiRu-1)封装在脱铁铁蛋白(AFt)纳米笼内的效果进行了研究。通过紫外/可见光谱、ICP-MS、CD 和 X 射线晶体学对 DiRu-1-AFt 纳米载体进行了表征。与之前报道的基于 Au 和 Pt 的载药 AFt 载体不同,我们没有发现 DiRu-1 与 AFt 之间存在直接相互作用的证据。DiRu-1-AFt 对 SV40 病毒(SVT2)转化的永生鼠 BALB/c-3T3 成纤维细胞和人表皮癌细胞 A431 具有细胞毒性,并对这些癌细胞具有中等选择性,而对正常 BALB/c-3T3 细胞则没有。DiRu-1-AFt 引发活性氧的产生、线粒体膜电位去极化,并通过 p53 介导的细胞凋亡诱导细胞死亡。与以前的结果相比,我们的数据表明,金属基药物与蛋白质笼内的 AFt 之间存在特定相互作用对于药物包封并不是必需的。
