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铬(III)与血管紧张素转换酶抑制剂卡托普利络合的实验与分子模拟研究

Experimental and Molecular Modeling Studies on the Complexation of Chromium(III) with the Angiotensin-Converting Enzyme Inhibitor Captopril.

作者信息

Mahmoud Shimaa A, Taha Mohamed, Khaled Eman S H, Hassan Walid Hamdy, Abo El-Ela Fatma I, Abdel-Khalek Ahmed A, Mohamed Reham A

机构信息

Chemistry Department, Faculty of Science, Beni-Suef University, 62511 Beni-Suef, Egypt.

Materials Science and Nanotechnology Department, Faculty of Postgraduate Studies for Advanced Sciences, Beni-Suef University, 62511 Beni-Suef, Egypt.

出版信息

ACS Omega. 2022 Apr 28;7(18):15909-15918. doi: 10.1021/acsomega.2c00986. eCollection 2022 May 10.

Abstract

Captopril (CPT) is an inhibitor of angiotensin I converting enzyme, used as a medication for the treatment of people with high blood pressure, renal insufficiency, and cardiovascular diseases. It inhibits the angiogenesis process, vasoconstriction, and tumor metastasis. Some metal-captopril complexes exhibit antimicrobial activities. In the current work, the formation of the Cr-CPT complex was studied spectrophotometrically and potentiometrically in aqueous solution. Kinetics of Cr-CPT complex formation was spectrophotometrically studied over the pH range 3.20-4.20, at an ionic strength of 0.3 M at 30-50 °C. Cr-CPT complex formation was potentiometrically studied at 25 °C, where ligand protonation constants and complexes' overall stability constants were calculated. UV-vis absorption spectra were executed to confirm the complex formation. Density functional theory and molecular dynamics simulation were performed to search the geometries of the Cr-CPT complex. Atoms in molecules and interaction region indicator calculations are used to investigate intermolecular interactions for the formation of Cr-CPT complex. The antimicrobial activity of the CPT ligand and Cr-CPT complex on the prevention and control of environmental pathogenic bacteria, as tested on both Gram-positive () and Gram-negative bacteria () via agar disc diffusion method, assess the ability to use as an antimicrobial agent. CPT had shown good antimicrobial activity against both types of bacteria, which had increased slightly the zone of inhibition in Cr-CPT that indicates the increased efficacy due to Cr(III) antimicrobial activity via its oxidative damage to the bacterial cell wall. No previous study tested the CPT antimicrobial activity against Gram-positive ones such as .

摘要

卡托普利(CPT)是一种血管紧张素I转换酶抑制剂,用作治疗高血压、肾功能不全和心血管疾病患者的药物。它抑制血管生成过程、血管收缩和肿瘤转移。一些金属 - 卡托普利配合物具有抗菌活性。在当前工作中,采用分光光度法和电位滴定法研究了水溶液中Cr - CPT配合物的形成。在30 - 50 °C、离子强度为0.3 M的条件下,在pH范围3.20 - 4.20内,采用分光光度法研究了Cr - CPT配合物形成的动力学。在25 °C下采用电位滴定法研究了Cr - CPT配合物的形成,计算了配体质子化常数和配合物的总稳定常数。通过紫外 - 可见吸收光谱证实了配合物的形成。进行了密度泛函理论和分子动力学模拟以探究Cr - CPT配合物的几何结构。利用分子中的原子和相互作用区域指示剂计算来研究形成Cr - CPT配合物的分子间相互作用。通过琼脂平板扩散法对CPT配体和Cr - CPT配合物对革兰氏阳性菌( )和革兰氏阴性菌( )的环境病原菌防控的抗菌活性进行测试,评估其作为抗菌剂的使用能力。CPT对两种类型的细菌均表现出良好的抗菌活性,在Cr - CPT中抑菌圈略有增加,这表明由于Cr(III)通过对细菌细胞壁的氧化损伤而具有抗菌活性,从而提高了疗效。此前没有研究测试过CPT对革兰氏阳性菌如 的抗菌活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/abea/9096923/b86f5c539586/ao2c00986_0001.jpg

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