Department of Chemical, Biological, Pharmaceutical and Environmental Sciences, University of Messina, 98166 Messina, Italy.
Department of Pharmaceutical Biology, Institute of Pharmaceutical and Biomedical Sciences, Johannes Gutenberg University, 55128 Mainz, Germany.
Molecules. 2022 Dec 17;27(24):9000. doi: 10.3390/molecules27249000.
Transition metal complexes have continued to constitute an appealing class of medicinal compounds since the exceptional discovery of cisplatin in the late 1960s. Pt(II)-based complexes are endowed with a broad range of biological properties, which are mainly exerted by targeting DNA. In this study, we report a significant biological investigation into and computation analyses of four Pt(II)-complexes, namely, , synthesized and characterized according to previously reported procedures. Molecular-modelling studies highlighted that the top two compounds (i.e., and ) might bind to both matched and mismatched base pair sites of the oligonucleotide 5'-(dCGGAAATTACCG)-3', supporting their anticancer potential. These two complexes displayed noteworthy cytotoxicity in vitro (sub-micromolar-micromolar range) against two leukaemia cell lines, i.e., CCRF-CEM and its multi-drug-resistant counterpart CEM/ADR5000, and remarkable anti-angiogenic properties (in the sub-micromolar range) evaluated in an in vivo model, i.e., a chick embryo chorioallantoic membrane (CAM) assay.
自 20 世纪 60 年代末顺铂这一非凡发现以来,过渡金属配合物一直是一类极富吸引力的药用化合物。Pt(II)配合物具有广泛的生物学特性,主要通过靶向 DNA 发挥作用。在这项研究中,我们对根据先前报道的程序合成和表征的四种 Pt(II)配合物,即 、 、 、 进行了深入的生物学研究和计算分析。分子建模研究强调,前两种化合物(即 和 )可能与寡核苷酸 5'-(dCGGAAATTACCG)-3'的匹配和不匹配碱基对位点都结合,这支持了它们的抗癌潜力。这两种配合物在体外对两种白血病细胞系(CCRF-CEM 和其多药耐药对应物 CEM/ADR5000)表现出显著的细胞毒性(亚微摩尔-微摩尔范围),并在体内模型(鸡胚绒毛尿囊膜(CAM)试验)中表现出显著的抗血管生成特性(亚微摩尔范围)。
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