In-Silico Prediction of Phytoconstituents from Manilkara Hexandra for Antidiabetic Activity Targeting GKRP (Glucokinase Regulatory Protein)

IF 0.1 Q4 MEDICINE, RESEARCH & EXPERIMENTAL International Journal of Ayurvedic Medicine Pub Date : 2023-07-03 DOI:10.47552/ijam.v14i2.3524
Apeksha P Motghare, Parimal P. KATOLKAR, Tina S Lichade
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Abstract

Objective: A complex metabolic condition known as diabetes mellitus is caused by either inadequate or dysfunctional insulin. Once more, medicinal plants are being researched for the treatment of diabetes. Prototypical compounds found in medicinal plants have been the source of many conventional medications. The part of our investigation was to test the phytoconstituents of Manilkara hexandra for antidiabetic efficacy, in-silico. Methods: The pattern of interaction between the phytoconstituents from the Manilkara hexandra (Roxb.) Dubard, plant and the crystal structure of the antidiabetic proteins is evaluated using molecular docking in Discovery Studio (PDB ID: 4LY9). Later, SwissADME and pkCSM were used to screen for toxicity as well as the pharmacokinetic profile. Results: The docked results suggest that quercetin (-9.3 kcal/mol), kaempferol (-9.1 kcal/mol), p-coumaric acid (-6.4 kcal/mol) and cinnamic acid (-6.3 kcal/mol) for 4LY9 macromolecule has best binding towards antidiabetic activity as compared to the standard drug metformin (-5.0 kcal/mol). According to ADMET tests, pharmacokinetics and toxicity characteristics were also within acceptable bounds. Conclusion: Results from the binding potential of phytoconstituents aimed at antidiabetic activity were encouraging. It promotes the usage of Manilkara hexandra and offers crucial details on pharmaceutical research and clinical care. 
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糖激酶调控蛋白(GKRP)抗糖尿病活性的芯片预测
目的:糖尿病是一种复杂的代谢疾病,由胰岛素不足或功能失调引起。再一次,药用植物被研究用于治疗糖尿病。在药用植物中发现的原型化合物是许多传统药物的来源。我们的研究的一部分是测试六合戟的植物成分的抗糖尿病功效,在硅。方法:对六芒罗各成分的相互作用规律进行研究。利用Discovery Studio (PDB ID: 4LY9)中的分子对接技术对Dubard、植物和抗糖尿病蛋白的晶体结构进行了评估。随后,使用SwissADME和pkCSM筛选毒性和药代动力学特征。结果:与标准药物二甲双胍(-5.0 kcal/mol)相比,槲皮素(-9.3 kcal/mol)、山奈酚(-9.1 kcal/mol)、对香豆酸(-6.4 kcal/mol)和肉桂酸(-6.3 kcal/mol)对4LY9大分子的抗糖尿病活性结合效果最好。根据ADMET试验,药代动力学和毒性特性也在可接受范围内。结论:植物成分结合电位对抗糖尿病活性的研究结果令人鼓舞。它促进了Manilkara hexandra的使用,并提供了药物研究和临床护理的关键细节。
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来源期刊
International Journal of Ayurvedic Medicine
International Journal of Ayurvedic Medicine MEDICINE, RESEARCH & EXPERIMENTAL-
自引率
50.00%
发文量
87
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