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具有各种吡啶连接桥联配体的双核 Pt(II) 配合物的新型小沟覆盖 DNA 结合模式及双重抗癌-抗血管生成活性。

New minor groove covering DNA binding mode of dinuclear Pt(II) complexes with various pyridine-linked bridging ligands and dual anticancer-antiangiogenic activities.

机构信息

Faculty of Science, Department of Chemistry, University of Kragujevac, R. Domanovića 12, 34000, Kragujevac, Serbia.

Faculty of Medical Sciences, Department of Pharmacy, University of Kragujevac, Svetozara Markovića 69, 34000, Kragujevac, Serbia.

出版信息

J Biol Inorg Chem. 2020 May;25(3):395-409. doi: 10.1007/s00775-020-01770-7. Epub 2020 Mar 11.

DOI:10.1007/s00775-020-01770-7
PMID:32162071
Abstract

New anticancer platinum(II) compounds simultaneously targeting tumor cells and tumor-derived neoangiogenesis, with new DNA interacting mode and large therapeutic window are appealing alternative to improve efficacy of clinical platinum chemotherapeutics. Herein, we describe three novel dinuclear [{Pt(en)Cl}(μ-L)] complexes with different pyridine-like bridging ligands (L), 4,4'-bipyridine (Pt1), 1,2-bis(4-pyridyl)ethane (Pt2) and 1,2-bis(4-pyridyl)ethene (Pt3), which highly, positively charged aqua derivatives, [{Pt(en)(HO)}(μ-L)], interact with the phosphate backbone forming DNA-Pt adducts with an unique and previously undescribed binding mode, called a minor groove covering. The results of this study suggested that the new binding mode of the aqua-Pt(II) complexes with DNA could be attributed to the higher anticancer activities of their chloride analogues. All three compounds, particularly complex [{Pt(en)Cl}(μ-4,4'-bipy)]Cl·2HO (4,4'-bipy is 4,4'-bipyridine) (Pt1), overcame cisplatin resistance in vivo in the zebrafish-mouse melanoma xenograft model, showed much higher therapeutic potential than antiangiogenic drug sunitinib malate, while effectively blocking tumor neovascularization and melanoma cell metastasis. Overall therapeutic profile showed new dinuclear Pt(II) complexes could be novel, effective and safe anticancer agents. Finally, the correlation with the structural characteristics of these complexes can serve as a useful tool for developing new and more effective anticancer drugs.

摘要

同时针对肿瘤细胞和肿瘤衍生新血管生成的新型抗癌铂(II)化合物,具有新的 DNA 相互作用模式和较大的治疗窗口,是改善临床铂类化疗疗效的一种有吸引力的替代方法。本文描述了三种新型双核 [{Pt(en)Cl}(μ-L)] 配合物,具有不同的吡啶类似桥联配体(L),4,4'-联吡啶(Pt1),1,2-双(4-吡啶基)乙烷(Pt2)和 1,2-双(4-吡啶基)乙烯(Pt3),它们是高度正电荷的水合衍生物,[{Pt(en)(HO)}(μ-L)],与磷酸骨架相互作用,形成具有独特且以前未描述的结合模式的 DNA-Pt 加合物,称为小沟覆盖。该研究结果表明,水合铂(II)配合物与 DNA 的新结合模式可归因于其氯化类似物更高的抗癌活性。三种化合物,特别是复合物 [{Pt(en)Cl}(μ-4,4'-bipy)]Cl·2HO(4,4'-bipy 是 4,4'-联吡啶)(Pt1),在斑马鱼-小鼠黑素瘤异种移植模型中克服了体内顺铂耐药性,表现出比抗血管生成药物舒尼替尼马来酸盐更高的治疗潜力,同时有效阻断肿瘤新生血管形成和黑素瘤细胞转移。总体治疗概况表明,新型双核 Pt(II) 配合物可能是新型、有效和安全的抗癌药物。最后,与这些配合物的结构特征的相关性可以作为开发新的、更有效的抗癌药物的有用工具。

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