Y. Magaji, Z. Abdullahi, A. Haroun, A. I. Alhaji, A. M. Sani
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The docking was done using a docking software between all the ligands and the target protein receptors. Natural compounds, such as Conduritol A, Catechin and Quercetin were picked, and protein targets as α-amylase and α-glucosidase. Ligands were imported for visual screening into PyRx software while Biovia Discovery Studio Visualizer was used for protein preparation. Analysis of the properties of drug likeliness of the ligands was done via SwissADME online server according to Lipinski’s Rule of Five. Final docking analysis was done through AutoDockVina and Biovia Discovery Studio client 2020. Molecular docking analysis of the ligands Conduritol A, Catechin and Quercetin showed strong binding interaction with both α-amylase and α-glucosidase. The test revealed different binding affinities, hydrogen bond interactions, hydrophobicity, solvent accessibility surface (SAS), root mean square deviation lower bound (RMSD LB) and root mean square deviation upper bound (RMSD UB). Conduritol A was the strongest compound against the protein targets, with its low binding strength, according to the PyRx test and Lipinski 's Rule of Five. The same molecules were further docked, and the interactions were visualized under PyMol Via Biovia Discovery Studio. According to the in silico study, we have found that these natural compounds can inhibit the activities of α-amylase and α-glucosidase which can be promising drugs for the treatment of diabetes after subjecting them to in vitro and in vivo studies.","PeriodicalId":14990,"journal":{"name":"Journal of Applied Life Sciences International","volume":"14 1","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2022-06-25","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Structure Based Docking of Secondary Metabolites against Alpha-amylase and Alpha-glucosidase Activities in Treating Diabetes\",\"authors\":\"Y. Magaji, Z. 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引用次数: 0
摘要
糖尿病(DM)是一种以胰岛素分泌不足、胰岛素抵抗或两者兼而有之导致高血糖(高血糖症)以及脂质、蛋白质和碳水化合物代谢不良为特征的长期代谢紊乱。这些并发症的发生是由于调节系统的葡萄糖储存和代谢燃料动员的紊乱,包括碳水化合物、蛋白质和脂质合成代谢和胰岛素分泌受损引起的分解代谢,或两者兼而有之。通过分子对接的方法,通过药物分子抑制α-淀粉酶和α-葡萄糖苷酶的活性来治疗糖尿病。所有的研究都是基于分子对接。对接是使用对接软件在所有配体和目标蛋白质受体之间完成的。天然化合物如孔雀糖醇A、儿茶素和槲皮素,蛋白质靶点为α-淀粉酶和α-葡萄糖苷酶。将配体导入PyRx软件进行视觉筛选,使用Biovia Discovery Studio Visualizer进行蛋白质制备。根据Lipinski的五法则,通过SwissADME在线服务器对配体的药物可能性进行分析。最后的对接分析是通过AutoDockVina和Biovia Discovery Studio客户端2020完成的。配体孔雀糖醇A、儿茶素和槲皮素与α-淀粉酶和α-葡萄糖苷酶均有较强的结合作用。实验结果显示了不同的结合亲和度、氢键相互作用、疏水性、溶剂可及性表面(SAS)、均方根偏差下界(RMSD LB)和均方根偏差上界(RMSD UB)。根据PyRx测试和Lipinski的五法则,Conduritol A是对蛋白质目标最强的化合物,其结合强度低。将相同的分子进一步对接,并在PyMol Via Biovia Discovery Studio下对相互作用进行可视化。通过体外和体内研究,我们发现这些天然化合物可以抑制α-淀粉酶和α-葡萄糖苷酶的活性,有望成为治疗糖尿病的有前途的药物。
Structure Based Docking of Secondary Metabolites against Alpha-amylase and Alpha-glucosidase Activities in Treating Diabetes
Diabetes mellitus (DM) is a long term disorder of metabolism characterized by high level of blood sugar (hyperglycemia) due to insufficient secretion of insulin, insulin resistance, or both, as well as poor lipid, protein and carbohydrate metabolism. These complications occur as a result of derangement in glucose storage for the regulatory system and metabolic fuel mobilization, including carbohydrate, protein and lipid anabolism and catabolism emanating from impaired action of insulin, secretion of insulin, or both. The in silico study was conducted with the help of molecular docking to treat diabetes to inhibit the activities of α-amylase and α-glucosidase by drug molecule. All the studies were based on docking with molecules. The docking was done using a docking software between all the ligands and the target protein receptors. Natural compounds, such as Conduritol A, Catechin and Quercetin were picked, and protein targets as α-amylase and α-glucosidase. Ligands were imported for visual screening into PyRx software while Biovia Discovery Studio Visualizer was used for protein preparation. Analysis of the properties of drug likeliness of the ligands was done via SwissADME online server according to Lipinski’s Rule of Five. Final docking analysis was done through AutoDockVina and Biovia Discovery Studio client 2020. Molecular docking analysis of the ligands Conduritol A, Catechin and Quercetin showed strong binding interaction with both α-amylase and α-glucosidase. The test revealed different binding affinities, hydrogen bond interactions, hydrophobicity, solvent accessibility surface (SAS), root mean square deviation lower bound (RMSD LB) and root mean square deviation upper bound (RMSD UB). Conduritol A was the strongest compound against the protein targets, with its low binding strength, according to the PyRx test and Lipinski 's Rule of Five. The same molecules were further docked, and the interactions were visualized under PyMol Via Biovia Discovery Studio. According to the in silico study, we have found that these natural compounds can inhibit the activities of α-amylase and α-glucosidase which can be promising drugs for the treatment of diabetes after subjecting them to in vitro and in vivo studies.
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