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首页> 外文期刊>Inorganica Chimica Acta >Bis- and mixed-ligand copper(II) complexes of nalidixic acid the antibacterial drug: Mode of nalidixate coordination determines DNA binding and cleavage and cytotoxicity
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Bis- and mixed-ligand copper(II) complexes of nalidixic acid the antibacterial drug: Mode of nalidixate coordination determines DNA binding and cleavage and cytotoxicity

机译:脱硫酸的双和混合配体铜(II)络合物抗菌药物:脱硫协调的模式决定了DNA结合和切割和细胞毒性

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摘要

The new complexes [Cu(nal)(2)]center dot 2H(2)O 1 and [Cu(en)(2)(nal)(2)] 2, where H(nal) is the antibacterial drug nalidixic acid, have been isolated and their X-ray structures successfully determined. The complex 1 possesses a square planar CuO4 chromophore constituted by the pyridone and carboxylate oxygen atoms of nalidixate anion. Complex 2 contains a CuN4O2 chromophore with a tetragonally distorted octahedral geometry, and the transaxial coordination of two nalidixate anions at longer distances to the CuN4 plane constituted by ethylenediamine is stabilized by a network of H-bonding. DFT studies illustrate the structures and stabilities of complexes. The DNA binding affinity of 2 (K-b, 9.2 (+/- 0.2) x 10(4) M-1) is higher than that of [Cu(en)(2)](2+) [K-b, 2.0 (+/- 0.2) x 10(4) M-1], illustrating that bound nal(-) enhances the DNA binding affinity. DNA docking studies reveal that 2 bound to DNA undergoes interesting coordinative distortions more than 1, causing more significant changes in DNA host. Thus, 2 displays oxidative DNA cleavage (ascorbic acid) more prominent than [Cu (en)(2)](2+), by generating (OH)-O-center dot radicals, and shows poor cytotoxicity towards A549 lung cancer cell lines.
机译:新复合物[Cu(nal)(2)]中心点2h(2)o 1和[Cu(en)(2)(nal)(2)] 2,其中H(nal)是抗菌药物脱硫酸,已被隔离,并成功确定了X射线结构。复合物1具有由吡啶酮和羧酸氧原子的正方形平面CuO4发色团,其脱硫阴离子。复合物2含有四边形变形的八面体几何形状的CUN4O2发色团,并且通过H键合网络稳定到与乙二胺构成的CUN4平面更长的距离距离的两个脱水阴离子的横向协调。 DFT研究说明了复合物的结构和稳定性。 2(kb,9.2(+/- 0.2)×10(4)m-1)的DNA结合亲和力高于[Cu(烯)(2)](2 +)[Kb,2.0(+ / - 0.2)×10(4)M-1],说明结合的NAL( - )增强DNA结合亲和力。 DNA对接研究表明,2与DNA结合经历有趣的协调扭曲超过1,导致DNA宿主的更大变化。因此,2显示氧化DNA裂解(抗坏血酸)比[Cu(Zh)(2)](2+),通过产生(OH)-O-中心点基团,并向A549肺癌细胞系显示细胞毒性差。

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