单溴和二溴取代席夫碱配合物镍(Ii)和锌(Ii)的合成、表征和生物学研究

Bussaba Pinchaipat, Teerawat Khudkham, S. Wongsuwan, Ratanon Chotima, K. Chainok, T. Pila
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引用次数: 0

摘要

合成了镍(II)和锌(II)与5-溴-N -(8-喹啉基)水杨醛二胺(HqsalBr, HL 1)和3,5-二溴-N -(8-喹啉基)水杨醛二胺(HqsalBr 2, HL 2)的过渡金属配合物,并利用IR、1h - nmr、质谱和热重分析(TGA)等技术成功地进行了表征。采用单晶x射线晶体学方法测定了镍(II)和锌(II)与hl2配合物的分子结构。配体hl1和hl2均为三齿配体,通过去质子化羟基氧原子、亚甲基官能团的氮和喹啉取代基的氮与金属离子中心配位。利用小牛胸腺DNA (CT-DNA)研究了这些复合物与DNA的相互作用,通过电子吸收和发光滴定的研究表明,这些复合物的DNA结合模式是插层的。所有合成的配合物都具有较大的结合常数(K b),这些结果与猝灭常数(K q)定义的猝灭能力一致。在合成的配合物中,锌(II)与配体HL 2配合物[Zn(qsalBr) 2]与CT-DNA的相互作用能力最强,与溴化乙啶(EB)的竞争反应验证模式也表明该配合物的插层性最强。此外,还研究了配体和配合物对A549细胞株的抗肺癌活性,并与标准化合物、依托泊苷和顺铂进行了比较。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Synthesis, Characterization and Biological Studies of Nickel ( Ii) and Zinc ( Ii) Complexes with Mono - and Di - Bromo Substituted Schiff Base Ligands
Transition metal complexes of nickel(II) and zinc(II) with 5-bromo- N -(8-quinolyl)salicylaldimine (HqsalBr, HL 1 ) and 3,5-dibromo- N -(8-quinolyl)salicylaldimine (HqsalBr 2 , HL 2 ) have been synthesized and successfully characterized using several techniques: IR, 1 H-NMR, mass spectrometry and thermogravimetric analysis (TGA). The molecular structures of nickel(II) and zinc(II) complexes with HL 2 were determined by single crystal X-Ray crystallography. Ligands HL 1 and HL 2 both act as a tridentate ligand and coordinate to metal ion center via deprotonated hydroxyl oxygen atom, nitrogen of azomethine functional group and nitrogen of quinoline substituent. The interaction of these complexes with DNA was investigated using calf thymus DNA (CT-DNA) in which the studies by electronic absorption and luminescence titrations reveal that DNA binding mode of the complexes is intercalation. All the synthesized complexes provide great values of binding constant (K b ) and these results are consistent with the quenching capability defined by quenching constant values (K q ). Amongst the synthesized complexes, zinc(II) with ligand HL 2 complex, [Zn(qsalBr) 2 ], exhibits the most superior ability in the interaction with CT-DNA and the verification mode of binding by the competitive reaction with ethidium bromide (EB) also indicates the strongest intercalation by such complex. Additionally, ligands and complexes were also examined in anti-lung cancer activity against A549 cell line and compared with standard compounds, Etoposide and Cisplatin.
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