Enisa Selimović, A. Komolkin, A. Egorov, T. Soldatović
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Copper(II) complexes offer various potential advantages as antimicrobial, antiviral, anti-inflammatory, antitumor agents, enzyme inhibitors, chemical nucleases, and they are also beneficial against several diseases like copper rheumatoid and gastric ulcers (Fricker, S.P., Dalton Trans. 2007, 43, 4903-4917).\nSubstitution reactions of square-planar [CuCl2(en)] and square-pyramidal [CuCl2(terpy)] complexes (where en= 1,2-diaminoethane and terpy= 2,2’:6’,2’’- terpyridine) with bio-relevant nucleophiles have been investigated at pH 7.4 in the presence of 0.010 M NaCl. Mechanism of substitution was probed via mole-ratio, kinetic, mass spectroscopy and EPR studies. In the presence of an excess of chloride, the octahedral complex anion [CuCl4(en)]2- forms rapidly while equilibrium reaction was observed for [CuCl2(terpy)]. Different order of reactivity of selected bio-molecules toward Cu(II) complexes was observed. The nature of the buffer just affects the Cu(II) complexes conformational dynamics. According to EPR data L-Methionine forms a most stable complex with [CuCl2(en)] among the bio-ligands considered while [CuCl2(terpy)] complex is very stable and there are no significant changes in its square-pyramidal geometry in the presence of buffers or bio-ligands. The obtained results represent progress in investigation of the mechanism of substitution reactions between Cu(II) complexes and biological relevant nuclepohiles. Also, they provide very useful information for the future design of potential copper-based anticancer drugs (Selimovic, E., et al. J. Coord. 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引用次数: 0
摘要
在过去的几十年里,过渡金属配合物在药物无机化学中引起了相当大的关注,特别是作为在生理条件下能够与DNA结合的合成金属核酸酶和金属基抗癌药物(Pessoa, J.C等)。j . Inorg。生物化学,2011,5,637-644)。铜(II)配合物在抗菌、抗病毒、抗炎、抗肿瘤、酶抑制剂、化学核酸酶等方面具有多种潜在优势,并且对铜类风湿性关节炎和胃溃疡等多种疾病也有益处(Fricker, S.P, Dalton Trans. 2007, 43, 4903-4917)。研究了方形平面[CuCl2(en)]和方形锥体[CuCl2(terpy)]配合物(其中en= 1,2-二氨基乙烷,terpy= 2,2′:6′,2′-三吡啶)与生物相关亲核试剂在pH 7.4、0.010 M NaCl存在下的取代反应。通过摩尔比、动力学、质谱和EPR研究对取代机理进行了探讨。在过量氯离子存在的情况下,八面体阴离子络合物[CuCl4(en)]2-迅速形成,而[CuCl2(terpy)]则观察到平衡反应。所选生物分子对Cu(II)配合物的反应性有不同的顺序。缓冲液的性质只影响Cu(II)配合物的构象动力学。根据EPR数据,在考虑的生物配体中,l -蛋氨酸与[CuCl2(en)]形成最稳定的配合物,而[CuCl2(terpy)]配合物非常稳定,并且在缓冲液或生物配体存在下其方锥体几何形状没有明显变化。这些结果代表了Cu(II)配合物与生物相关亲核试剂之间取代反应机理的研究进展。此外,它们为未来设计潜在的铜基抗癌药物提供了非常有用的信息(Selimovic, E., et al.)。[j] .化学学报,2018,71(7),1003-1019。
Impact of different geometrical structures of copper(II) complexes on interactions with bio-relevant nucleophiles under physiological conditions
Over the past decades, transition metal complexes have attracted considerable attention in medicinal inorganic chemistry, especially as synthetic metallonucleases and metal-based anticancer drugs that are able to bind to DNA under physiological conditions (Pessoa, J.C., et al. J. Inorg. Biochem. 2011, 105, 637-644). Copper(II) complexes offer various potential advantages as antimicrobial, antiviral, anti-inflammatory, antitumor agents, enzyme inhibitors, chemical nucleases, and they are also beneficial against several diseases like copper rheumatoid and gastric ulcers (Fricker, S.P., Dalton Trans. 2007, 43, 4903-4917).
Substitution reactions of square-planar [CuCl2(en)] and square-pyramidal [CuCl2(terpy)] complexes (where en= 1,2-diaminoethane and terpy= 2,2’:6’,2’’- terpyridine) with bio-relevant nucleophiles have been investigated at pH 7.4 in the presence of 0.010 M NaCl. Mechanism of substitution was probed via mole-ratio, kinetic, mass spectroscopy and EPR studies. In the presence of an excess of chloride, the octahedral complex anion [CuCl4(en)]2- forms rapidly while equilibrium reaction was observed for [CuCl2(terpy)]. Different order of reactivity of selected bio-molecules toward Cu(II) complexes was observed. The nature of the buffer just affects the Cu(II) complexes conformational dynamics. According to EPR data L-Methionine forms a most stable complex with [CuCl2(en)] among the bio-ligands considered while [CuCl2(terpy)] complex is very stable and there are no significant changes in its square-pyramidal geometry in the presence of buffers or bio-ligands. The obtained results represent progress in investigation of the mechanism of substitution reactions between Cu(II) complexes and biological relevant nuclepohiles. Also, they provide very useful information for the future design of potential copper-based anticancer drugs (Selimovic, E., et al. J. Coord. Chem. 2018, 71(7), 1003-1019).
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