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首页> 外文期刊>RSC Advances >Two new mixed copper(II)-dipeptide complexes of N,N-donor heterocycle ligands: studies on their non-covalent DNA binding, chemical nuclease, antioxidant and anticancer activities
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Two new mixed copper(II)-dipeptide complexes of N,N-donor heterocycle ligands: studies on their non-covalent DNA binding, chemical nuclease, antioxidant and anticancer activities

机译:N,N-供体杂环配体的两种新的混合铜(II)-二肽配合物:它们的非共价DNA结合,化学核酸酶,抗氧化剂和抗癌活性的研究

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Two novel mononuclear mixed ligand copper(II) complexes, [Cu(Gly-L-val)(HPB)(H2O)]center dot ClO4 center dot 1.5H(2)O (1) and [Cu(Gly-L-val)(PBT)(H2O)]center dot ClO4 (2) (Gly-L-val = glycyl-L-valine, HPB = 2-(2'-pyridyl) benzimidazole, PBT = 2-(2'-pyridyl) benzothiazole), have been synthesized and characterized using various analytical and spectroscopic methods. The interactions of the complexes with DNA have been explored by viscometry, thermal denaturation, cyclic voltammetry (CV), agarose gel electrophoresis and spectroscopic means (UV absorption, circular dichroism (CD) and fluorimetry), as well as molecular docking techniques. These studies confirmed the mode of the complexes bound to calf thymus DNA (CT-DNA) through insertion with certain affinity (K-b = 3.211 x 10(5) M-1 for 1 and 4.734 x 10(4) M-1 for 2). In the fluorimetric experiments of thermodynamics (K-SV = 1.145 x 10(4) M-1 for 1 and 2.634 x 10(3) M-1 for 2), the changes in enthalpy (Delta H > 0), entropy (Delta S > 0) and Gibbs free energy (Delta G < 0) in the interactions between the complexes with DNA suggested that the process occurred spontaneously through hydrophobic interactions. The complexes displayed oxidative cleavage of pBR322 plasmid DNA in the presence of ascorbic acid, probably induced by (OH)-O-center dot as a reactive oxygen species. Furthermore, the molecular docking technique was applied to ascertain the mode of action for the complexes towards DNA. Moreover, superoxide dismutase (SOD) activity studies were performed using the photoreduction of nitroblue tetrazolium (NBT) under a non-enzymatic system and the antioxidant activities of 1 and 2 determined with IC50 values of 0.337 and 0.146 mu M, respectively. The cytotoxicity of the Cu(II) complexes against A549, HeLa, PC-3 tumor cell lines and NIH3T3 (non-tumor cell line) was studied by an MTT assay and it was found that 1 exhibited better cytotoxicity against A549 and PC-3 than 2 and the widely used drug cisplatin.
机译:两种新型单核混合配体铜(II)配合物,[Cu(Gly-L-val)(HPB)(H2O)]中心点ClO4中心点1.5H(2)O(1)和[Cu(Gly-L-val )(PBT)(H2O)]中心点ClO4(2)(Gly-L-val =缩水甘油基-L-缬氨酸,HPB = 2-(2'-吡啶基)苯并咪唑,PBT = 2-(2'-吡啶基)苯并噻唑),已使用各种分析和光谱方法进行了合成和表征。已通过粘度测定,热变性,循环伏安法(CV),琼脂糖凝胶电泳和光谱学方法(紫外线吸收,圆二色性(CD)和荧光法)以及分子对接技术研究了配合物与DNA的相互作用。这些研究证实了通过以一定亲和力插入而与小牛胸腺DNA(CT-DNA)结合的复合物的模式(Kb = 3.211 x 10(5)M-1代表1和4.734 x 10(4)M-1代表2) 。在热力学的荧光实验中(K-SV = 1.145 x 10(4)M-1(1)和2.634 x 10(3)M-1(2)),焓变(Delta H> 0),熵(Delta S> 0)和吉布斯自由能(Delta G <0)在复合物与DNA之间的相互作用中表明该过程是通过疏水相互作用自发发生的。该复合物在抗坏血酸的存在下显示pBR322质粒DNA的氧化裂解,这可能是由(OH)-O-中心点作为活性氧引起的。此外,应用了分子对接技术来确定复合物对DNA的作用方式。此外,超氧化物歧化酶(SOD)活性的研究是在非酶系统下使用硝基蓝四唑(NBT)的光还原,并通过IC50值分别为0.337和0.146μM来确定1和2的抗氧化活性。通过MTT分析研究了Cu(II)配合物对A549,HeLa,PC-3肿瘤细胞系和NIH3T3(非肿瘤细胞系)的细胞毒性,发现1对A549和PC-3具有更好的细胞毒性。比2和广泛使用的药物顺铂。

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