Laboratory of Inorganic Chemistry, Department of Chemistry, Aristotle University of Thessaloniki, Thessaloniki 54124, Greece.
Laboratory of Pharmacology, Medical School, National and Kapodistrian University of Athens, 75 Mikras Asias Street, Athens 11527, Greece.
J Inorg Biochem. 2022 Mar;228:111695. doi: 10.1016/j.jinorgbio.2021.111695. Epub 2021 Dec 29.
A series of heteroleptic Ag(I) complexes bearing 4,6-dimethyl-2-pyrimidinethiol (dmp2SH), i.e., [AgCl(dmp2SH)(PPh)] (1), [Ag(dmp2SH)(PPh)]NO (2), [Ag(dmp2SΗ)(xantphos)]NO (3), [Ag(μ-dmp2S)(PPh)] (4), [Ag(dmp2S)(xantphos)] (5), [Ag(μ-dmp2S)(DPEphos)] (6) (xantphos = 4,5-bis(diphenylphosphino)-9,9-dimethylxanthene and DPEPhos = bis[(2-diphenylphosphino)phenyl]ether) were synthesized. The complexes display systematic variation of particular structural characteristics which were proved to have a significant impact on their in vitro cytotoxicity and antimicrobial properties. A moderate-to-high potential for bacteria growth inhibition was observed for all complexes, with 2, 3 and 5 being particularly effective against Gram-(+) bacteria (IC = 1.6-4.5 μM). The three complexes exhibit high in vitro cytotoxicity against HeLa and MCF-7 cancer cells (IC = 0.32-3.00 μΜ), suggesting the importance of coordination unsaturation and cationic charge for effective bioactivity. A very low cytotoxicity against HDFa normal cells was observed, revealing a high degree of selectivity (selectivity index ~10) and, hence, biocompatibility. Fluorescence microscopy using 2 showed effective targeting on the membrane of the HeLa cancer cells, subsequently inducing cell death. Binding of the complexes to serum albumin proteins is reasonably strong for potential uptake and subsequent release to target sites. A moderate in vitro antioxidant capacity for free radicals scavenging was observed and a low potential to destroy the double-strand structure of calf-thymus DNA by intercalation, suggesting likely implication of these properties in the bioactivity mechanisms of these complexes. Further insight into possible mechanisms of bioactivity was obtained by molecular modeling calculations, by exploring their ability to act as potential inhibitors of DNA-gyrase, human estrogen receptor alpha, human cyclin-dependent kinase 6, and human papillomavirus E6 oncoprotein.
一系列含有 4,6-二甲基-2-嘧啶硫醇(dmp2SH)的异双核银(I)配合物,即 [AgCl(dmp2SH)(PPh)](1)、[Ag(dmp2SH)(PPh)]NO(2)、[Ag(dmp2SΗ)(xantphos)]NO(3)、[Ag(μ-dmp2S)(PPh)](4)、[Ag(dmp2S)(xantphos)](5)、[Ag(μ-dmp2S)(DPEphos)](6)(xantphos=4,5-双(二苯基膦基)-9,9-二甲基氧杂蒽和 DPEPhos=双[(2-二苯基膦基)苯基]醚)被合成。这些配合物显示出特定结构特征的系统变化,这些变化被证明对它们的体外细胞毒性和抗菌性能有显著影响。所有配合物对细菌生长均具有中度至高的抑制潜力,其中 2、3 和 5 对革兰氏阳性菌(IC=1.6-4.5μM)特别有效。三种配合物对 HeLa 和 MCF-7 癌细胞的体外细胞毒性较高(IC=0.32-3.00μM),表明配位不饱和和阳离子电荷对有效生物活性的重要性。对 HDFa 正常细胞的细胞毒性非常低,显示出高度的选择性(选择性指数~10)和生物相容性。使用 2 的荧光显微镜显示了对 HeLa 癌细胞膜的有效靶向,随后诱导细胞死亡。配合物与血清白蛋白蛋白的结合对于潜在的摄取和随后释放到靶位是合理的强。观察到对自由基清除的适度体外抗氧化能力,以及通过嵌入破坏小牛胸腺 DNA 双链结构的低潜力,这表明这些性质可能参与了这些配合物的生物活性机制。通过分子建模计算进一步深入了解生物活性的可能机制,探索了它们作为 DNA-拓扑异构酶、人雌激素受体α、人细胞周期蛋白依赖性激酶 6 和人乳头瘤病毒 E6 癌蛋白潜在抑制剂的能力。
