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Antitumor activity and DNA binding studies on rare earth metal complexes with all-trans retinoic acid and L-glutamic acid

机译:全反式维甲酸和L-谷氨酸对稀土金属配合物的抗肿瘤活性和DNA结合研究

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Four new complexes have been synthesized by the reaction of rare earth (III) nitrate with all-trans retinoic acid as the first ligand and L-glutamic acid as the second ligand in an alcoholic solution (pH = 6.5-7.0) with the aim to develop new antitumor drugs. The composition of the complexes has been characterized by elemental analysis, molar conductivity, IR spectroscopy, H-1 NMR spectroscopy, thermogravimetric analysis and UV-vis methods. The general molecular formula of the complexes was determined to be REL2L' (RE = Nd, Eu, La, Sc, L = all-trans retinoic acid, L' = L-glutamic acid). The antitumor activities of complexes and corresponding ligands were tested by MTT methods. The results indicate that the four rare earth complexes possess different degrees of inhibiting effects on HepG2, A549 and HeLa cells. The suppression ratio of the complexes against the tested tumour cells is superior for the two ligands and RE(III) ions. Especially, the EuL2L' showed the most obvious antitumor activity on HepG2 and HeLa cells. To investigate the mechanism of inhibition of the complexes, EuL2L' reacting with DNA was studied by fluorescence spectra, viscosity, UV and CD spectra, and the results showed that the mode of interaction was mainly by intercalation, which may be the one of the important reasons for the highest antitumor activity of the EuL2L' complex. The results obtained in this study provide certain ideas and an experimental basis for the development of highly efficient and rare earth antitumor drugs that have low toxicity.
机译:硝酸稀土(III)与全反式视黄酸作为第一配体和L-谷氨酸作为第二配体在酒精溶液(pH = 6.5-7.0)中反应合成了四个新的配合物,目的是开发新的抗肿瘤药物。配合物的组成已通过元素分析,摩尔电导率,IR光谱,H-1 NMR光谱,热重分析和UV-vis方法进行了表征。确定该配合物的一般分子式为REL2L'(RE = Nd,Eu,La,Sc,L =全反式维甲酸,L'= L-谷氨酸)。通过MTT方法测试复合物和相应配体的抗肿瘤活性。结果表明,四种稀土配合物对HepG2,A549和HeLa细胞具有不同程度的抑制作用。对于两种配体和RE(III)离子,复合物对所测试的肿瘤细胞的抑制率更高。特别是EuL2L'对HepG2和HeLa细胞显示出最明显的抗肿瘤活性。为了研究复合物的抑制机理,通过荧光光谱,粘度,UV和CD光谱研究了EuL2L'与DNA的反应,结果表明相互作用的方式主要是通过嵌入,这可能是重要的原因之一。 EuL2L'复合物具有最高抗肿瘤活性的原因。本研究获得的结果为开发低毒的高效稀土抗肿瘤药物提供了一定的思路和实验依据。

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