Department of Chemistry, Aligarh Muslim University, Aligarh 202002, India.
Department of Chemistry, Aligarh Muslim University, Aligarh 202002, India.
J Photochem Photobiol B. 2017 Sep;174:106-125. doi: 10.1016/j.jphotobiol.2017.07.023. Epub 2017 Jul 24.
Synthesis of bio-efficient homobimetallic complexes, Cu(L)(dipic).3HO (1), Zn(L)(dipic).4HO (2), Cu(L)(oxa).4HO (3) and [Zn(L)(oxa)] (NO).5HO (4) was carried out using Schiff bases [(NE,NE)-N,N-bis(5-chlorothiophen-2-ylmethylene)-4-chlorobenzene-1,2-diamine; L] and [(NE,NE)-N,N-bis(5-chlorofuran-2-ylmethylene)-4-chlorobenzene-1,2-diamine; L] as main ligands and dicarboxylate moieties of 2,6-pyridine dicarboxylic acid (H-dipic) and oxalic acid (H-oxa) as co-ligands, respectively in order to apprehend their structure activity relationships on the basis of pharmacophore hybrid approach. The stoichiometry, geometry, thermal stability, morphology and crystallite size of the compounds were inferred by analytical, spectral (FT-IR, H NMR and C NMR and Mass), thermal (TGA/DTA), SEM and XRD studies. In-vitro DNA and HSA binding profiles of complexes were analysed by different biophysical measurements. The absorption study divulged that the observed alterations in the physico-chemical properties of complexes upon binding with DNA connoted their intercalative binding mode while fluorescence quenching mechanism was quantified by using Stern Volmer constant (K) 1.73×10 (1), 1.47×10 (2), 5.65×10 (3) and 3.60×10M (4) which discerned that hybrid pharmacophore active metal complexes (1 and 2) exhibited efficient quenching effect with Ct-DNA in comparison to complexes (3 and 4) due to greater planarity and extent of conjugation (π-π interactions). The intercalative binding mode of complexes is further supported by competitive displacement assay by using fluorogenic dyes (EtBr and Hoechst 33258). The results of HSA fluorescence study divulged static quenching of the complexes (1-4) with K values of 7.24×10 (1), 6.03×10 (2), 5.06×10 (3) and 2.85×10 (4) while K values; 1.16×10 (1), 2.01×10 (2), 5.84×10 (3) and 8.60×10 (4) suggested them potent avid binder of HSA. Additionally, comparative estimation of scavenging properties using DPPH, superoxide(O), hydroxyl (OH) and ABTS method and in-vitro cytotoxicity against different cell lines (MCF-7, HeLa and Hep G2) brought out distinct biopotency of complexes due to diverse structural features and chelation effect.
采用席夫碱[(NE,NE)-N,N-双(5-氯噻吩-2-亚甲基)-4-氯苯-1,2-二胺;L]和[(NE,NE)-N,N-双(5-氯呋喃-2-亚甲基)-4-氯苯-1,2-二胺;L]作为主配体,2,6-吡啶二甲酸(H-二吡啶)和草酸(H-氧杂)的二羧酸部分分别作为共配体,合成了生物有效的同双核配合物[Cu(L)(二吡啶)](NO 3 )·3H 2 O(1)、[Zn(L)(二吡啶)](NO 3 )·4H 2 O(2)、[Cu(L)(氧杂)](NO 3 )·4H 2 O(3)和[Zn(L)(氧杂)](NO 3 )·5H 2 O(4),以基于药效团杂合方法理解它们的结构-活性关系。通过分析、光谱(FT-IR、H NMR 和 C NMR 和质谱)、热(TGA/DTA)、SEM 和 XRD 研究推断了化合物的化学计量比、几何形状、热稳定性、形态和结晶度。通过不同的生物物理测量分析了配合物与 DNA 和 HSA 的结合特性。吸收研究表明,配合物与 DNA 结合时理化性质的观察到的变化表明它们具有插入结合模式,而荧光猝灭机制通过使用 Stern Volmer 常数(K)1.73×10(1)、1.47×10(2)、5.65×10(3)和 3.60×10(4)进行了定量,这表明杂药效团活性金属配合物(1 和 2)与 DNA 相比,由于更大的平面性和共轭程度(π-π 相互作用),具有更有效的荧光猝灭作用。通过使用荧光染料(EtBr 和 Hoechst 33258)进行竞争性置换测定,进一步支持了配合物的插入结合模式。HSA 荧光研究的结果表明,配合物(1-4)与 K 值为 7.24×10(1)、6.03×10(2)、5.06×10(3)和 2.85×10(4)发生静态猝灭,而 K 值;1.16×10(1)、2.01×10(2)、5.84×10(3)和 8.60×10(4)表明它们是 HSA 的有效结合物。此外,使用 DPPH、超氧化物(O )、羟基(OH)和 ABTS 方法进行清除性质的比较评估以及对不同细胞系(MCF-7、HeLa 和 Hep G2)的体外细胞毒性研究,由于不同的结构特征和螯合效应,揭示了配合物的明显生物功效。
