Interaction of metallocene dichlorides with apo-human transferrin: A spectroscopic study and cytotoxic activity against human cancer cell lines.

International journal of molecular biology (Edmond, Okla.) Pub Date : 2020-01-01 Epub Date: 2020-07-31
Jorge R Güette Fernández, Xiomara Narváez Pita, Enrique Meléndez, Elsie I Parés Matos
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Abstract

Metallocene dichlorides (Cp2M(IV)Cl2) are the first class of small and hydrophobic organometallic compounds classified as anticancer agents against numerous cancer cell lines and tumors. In this study, the antiproliferative activities of Cp2VCl2,Cp2NbCl2, Cp2HfCl2 and Cp2ZrCl2were assessed on two human cancer cell lines (HT-29 and MCF-7) using MTT assay. Spectroscopic studies were also conducted using these and other known metallocene dichlorides on apo-human transferrin (apo-hTf) at pH 7.4. UV-Vis and CD showed that their interaction with apo-hTf could induce conformational changes of its secondary structure during binding process. In fluorescence, a decrease in intensity of the emission peak was observed when the apo-hTf:Cp2M(IV)Cl2 complex is being formed, probably due to changes in the microenvironment of its tyrosine and tryptophan residues. Among all metallocene dichlorides studied, Cp2VCl2 has the strong ability to quench the intrinsic fluorescence of apo-hTf through a static quenching mechanism. The association constants for each protein-compound complex were also determined at different temperatures (296 K, 303 K, 310 K, and 317 K) based on fluorescence quenching results. Positive enthalpy changes (ΔH) and entropy changes (ΔS) as well as negative free energies (ΔG) suggest that hydrophobic interactions are the main intermolecular forces involved in the binding process, probably via an endothermic and spontaneous reaction mechanism. The distance, r, between donor (apo-hTf) and acceptor (Cp2M(IV)Cl2) obtained according to Forster's theory of non-radiation energy transfer suggest that the energy transfer from apo-hTf to Cp2M(IV)Cl2 occurs with high probability and distances obtained by FRET with high accuracy.

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茂金属二氯化物与载人转铁蛋白的相互作用:光谱研究和对人类癌细胞系的细胞毒性活性。
茂金属二氯化物(Cp2M(IV)Cl2)是一类小分子、疏水的有机金属化合物,被列为抗癌药物,可治疗多种癌细胞系和肿瘤。本研究采用MTT法测定了Cp2VCl2、Cp2NbCl2、Cp2HfCl2和cp2zrcl2对2种人癌细胞HT-29和MCF-7的抗增殖活性。用这些和其他已知的茂金属二氯化物对pH值为7.4的载人转铁蛋白(载铁htf)进行了光谱研究。UV-Vis和CD表明,它们与载脂蛋白htf的相互作用在结合过程中会引起其二级结构的构象变化。在荧光中,当apo-hTf:Cp2M(IV)Cl2复合物形成时,观察到发射峰强度降低,这可能是由于其酪氨酸和色氨酸残基的微环境发生了变化。在所研究的茂金属二氯化物中,Cp2VCl2通过静态猝灭机制猝灭apo-hTf的固有荧光。根据荧光猝灭结果,测定了不同温度(296 K、303 K、310 K和317 K)下每种蛋白-化合物复合物的缔合常数。正焓变(ΔH)和熵变(ΔS)以及负自由能(ΔG)表明疏水相互作用是参与结合过程的主要分子间作用力,可能是通过吸热自发反应机制进行的。根据Forster的非辐射能量转移理论得到的供体(apo-hTf)与受体(Cp2M(IV)Cl2)之间的距离r表明,apo-hTf向Cp2M(IV)Cl2的能量转移概率高,FRET得到的距离精度高。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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