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两种必需金属配合物的合成与结构解析:体外研究其与 BSA/HSA 的结合特性、对接模拟和抗癌活性。

Synthesis and Structure Elucidation of Two Essential Metal Complexes: In-Vitro Studies of Their BSA/HSA-Binding Properties, Docking Simulations, and Anticancer Activities.

机构信息

School of Chemical Engineering, Henan Technical Institute, Zhengzhou 450042, China.

School of Chemistry and Chemical Engineering, Henan University of Technology, Zhengzhou 450001, China.

出版信息

Molecules. 2022 Mar 14;27(6):1886. doi: 10.3390/molecules27061886.

Abstract

Imidazole and tetrazole derivatives are widely used as clinical drugs since they possess a variety of pharmaceutical function. Zinc and iron are essential trace elements of the human body, with less toxicity and good biocompatibility. In this paper, two new essential metal mononuclear complexes [M(Htmidc)(HO)]·2HO (M = Zn (), Fe ()) were synthesized through the reaction of 2-((1-tetrazol-1-yl)methylene)-1-imidazole-4,5-dicarboxylic acid (Htmidc) and ZnSO·7HO or FeSO·7HO. The crystal structures were determined by means of the X-ray single crystal diffraction technique. Results from fluorescence investigations show that both complexes could interact with BSA as well as HSA through the static quenching mechanism. van der Waals forces and hydrogen bonds play important roles in the interaction of complexes and BSA/HSA since both Δ and Δ values are negative. The results of molecular docking are consistent with those in experimental studies. Furthermore, the anticancer activity of Htmidc and both complexes against Eca-109 were preliminarily evaluated and the results show that both complexes have better anticancer activity than the corresponding ligand Htmidc.

摘要

咪唑和四唑衍生物由于具有多种药物功能,被广泛用作临床药物。锌和铁是人体必需的微量元素,具有较低的毒性和良好的生物相容性。本文通过 2-((1-四唑-1-基)亚甲基)-1-咪唑-4,5-二羧酸(Htmidc)与 ZnSO·7HO 或 FeSO·7HO 的反应,合成了两种新的必需金属单核配合物[M(Htmidc)(HO)]·2HO(M = Zn(),Fe())。通过 X 射线单晶衍射技术确定了晶体结构。荧光研究结果表明,两种配合物都可以通过静态猝灭机制与 BSA 和 HSA 相互作用。范德华力和氢键在配合物与 BSA/HSA 的相互作用中起重要作用,因为 Δ 和 Δ 值均为负值。分子对接的结果与实验研究一致。此外,还初步评价了 Htmidc 和两种配合物对 Eca-109 的抗癌活性,结果表明两种配合物的抗癌活性均优于相应配体 Htmidc。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4ce5/8948964/26ccc2d7ac0d/molecules-27-01886-sch001.jpg

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