Synthesis, Antimicrobial Activity, DFT, Molecular Docking, and Dynamic Simulations of Trityl Mannopyranoside Derivatives for Potential Antibacterial Agents.

IF 1.9 4区医学 Q3 CHEMISTRY, MEDICINAL Medicinal Chemistry Pub Date : 2025-01-02 DOI:10.2174/0115734064339243241027024304

Sabina Akter, Sarkar M A Kawsar, Gassoumi Bouzid, Mabrouk Horchani, Md Z H Bulbul, Houcine Ghalla, Hichem Ben Jannet, Supriyo Saha, Yuki Fujii, Kabir M Uddin, Ajmal R Bhat, Sumeer Ahmed, Yasuhiro Ozeki

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Abstract

Aim: There is an urgent need for new antimicrobial compounds with alternative modes of action for the treatment of drug-resistant bacterial and fungal pathogens.

Background: Carbohydrates and their derivatives are essential for biochemical and medicinal research because of their efficacy in the synthesis of biologically active drugs.

Objective: In the present study, a series of methyl α-D-mannopyranoside (MMP) derivatives (2-6) were prepared via direct acylation, and their biological properties were characterized.

Methods: The structures of synthesized compounds were established by analyzing their physicochemical, elemental, and spectroscopic data and evaluating their in vitro antimicrobial activities through in silico studies.

Results: In the antibacterial study, compound 3 was found to be mostly active toward most of the organisms, exhibiting maximum inhibition of S. abony and minimum inhibition of P. aeruginosa. However, the MIC and MBC values revealed that this compound is highly effective against Bacillus subtilis (MIC of 0.5 μg/L and MBC of 256 μg/L). In terms of antifungal activity, 3 and 6 showed the most promising activity toward Aspergillus flavus, with an inhibition of 95.90 ± 1.0% for compound 3 and 96.72 ± 1.1% for compound 6. Moreover, density functional theory (DFT) in conjunction with the BLYP/6-311G (d) basis sets was used to calculate the dipole moment and total energy for each compound, and the molecular electrostatic potential and Mulliken charge were considered to study the electrophilicity and nucleophilicity of the groups in each compound. For dipole moment calculations, the dipole moments are in the following order: 6 < 3 < 1 < 5 < 2 < 4, inferring that compounds 2 and 4 possess a high dipole moment in comparison with the other inhibitor systems. Furthermore, molecular docking was performed against threonine synthase from B. subtilis ATCC 6633 (PDB: 6CGQ) to identify the active site of the compounds, with compound 3 showing a maximum binding energy of -10.3 kcal/mol and compound 4 exhibiting a binding energy of -10.2 kcal/mol. In addition, a 100 ns MD simulation was performed, and the results revealed a stable conformation and binding pattern within the stimulating environment.

Conclusion: Our synthetic, antimicrobial, and in silico experiments revealed that MMP derivatives exhibit potential activity, providing a therapeutic target for bacteria and fungi.

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潜在抗菌剂三酰基甘露吡喃苷衍生物的合成、抗菌活性、DFT、分子对接和动态模拟。

目的：迫切需要具有替代作用模式的新型抗菌化合物来治疗耐药细菌和真菌病原体。背景：碳水化合物及其衍生物在生物活性药物的合成中具有重要作用，是生物化学和医学研究的重要组成部分。目的：通过直接酰化法制备一系列甲基α- d -甘露pyranoside （MMP）衍生物（2-6），并对其生物学特性进行表征。方法：通过理化、元素和波谱分析确定合成化合物的结构，并通过计算机实验对其体外抗菌活性进行评价。结果：在抗菌研究中，化合物3对大部分病原菌均有较强的抑菌活性，对S. abony的抑菌作用最大，对P. aeruginosa的抑菌作用最小。MIC和MBC测定结果表明，该化合物对枯草芽孢杆菌具有较好的抑菌活性（MIC为0.5 μg/L， MBC为256 μg/L）。在抗真菌活性方面，化合物3和6对黄曲霉的抑制率最高，分别为95.90±1.0%和96.72±1.1%。利用密度泛函理论（DFT）结合BLYP/6-311G (d)基集计算了每种化合物的偶极矩和总能量，并考虑了分子静电势和Mulliken电荷来研究每种化合物中基团的亲电性和亲核性。对于偶极矩计算，偶极矩的顺序为：6 < 3 < 1 < 5 < 2 < 4，推断化合物2和4与其他抑制剂体系相比具有较高的偶极矩。对枯草芽孢杆菌ATCC 6633 （PDB: 6CGQ）的苏氨酸合成酶进行分子对接，确定了化合物的活性位点，化合物3的最大结合能为-10.3 kcal/mol，化合物4的最大结合能为-10.2 kcal/mol。此外，进行了100 ns MD模拟，结果显示在刺激环境中具有稳定的构象和结合模式。结论：我们的合成、抗菌和硅实验表明，MMP衍生物具有潜在的活性，为细菌和真菌提供了治疗靶点。

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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来源期刊

Medicinal Chemistry 医学-医药化学

CiteScore

4.30

自引率

4.30%

发文量

109

审稿时长

12 months

期刊介绍： Aims & Scope Medicinal Chemistry a peer-reviewed journal, aims to cover all the latest outstanding developments in medicinal chemistry and rational drug design. The journal publishes original research, mini-review articles and guest edited thematic issues covering recent research and developments in the field. Articles are published rapidly by taking full advantage of Internet technology for both the submission and peer review of manuscripts. Medicinal Chemistry is an essential journal for all involved in drug design and discovery.