Docking study of allicin with sulfonylurea receptor 1, complex 1 and ppary receptor on insulin resistance
Publication details: M. P. Innovare Academic Sciences Pvt Ltd 2018Edition: Vol. 10(10), July-AugustDescription: 130-133Subject(s): Online resources: In: International journal of pharmacy and pharmaceutical scienceSummary: Objective: Allicin is a potential type 2 antidiabetic. Sulfonylurea receptor 1 (SUR1), nikotinamida adina dinukleotida dehydrogenase (Complex 1) and peroxisome proliferator-activated receptors gamma (PPARγ) are known as important receptors responsible in insulin resistance This study aimed to determine the physicochemical properties, and the affinity of allicin on SUR1, Complex 1 and PPARγ receptors based on the binding energy and the type of interaction. Methods:The physicochemical properties of allicin were analyzed using ChemOffice, and the binding energy and type of interaction were analyzed using the docking method with Autodock Vina. Results: The results from the analysisshowed allicin has log p (logarithmic partition) 1.35, massa relativity (mr) 162.26 g/mol, and the binding energy of allicin on SUR1, Complex 1 and PPARγ are respectively-4.0; -3.0; and-4.1 kcal/mol. The type of interactionbetween allicin and receptors is van der waals. Conclusion:Allicin has good....| Item type | Current library | Status | Barcode | |
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School of Pharmacy Archieval Section | Not for loan | 2018431 |
Objective: Allicin is a potential type 2 antidiabetic. Sulfonylurea receptor 1 (SUR1), nikotinamida adina dinukleotida dehydrogenase (Complex 1) and peroxisome proliferator-activated receptors gamma (PPARγ) are known as important receptors responsible in insulin resistance This study aimed to determine the physicochemical properties, and the affinity of allicin on SUR1, Complex 1 and PPARγ receptors based on the binding energy and the type of interaction. Methods:The physicochemical properties of allicin were analyzed using ChemOffice, and the binding energy and type of interaction were analyzed using the docking method with Autodock Vina. Results: The results from the analysisshowed allicin has log p (logarithmic partition) 1.35, massa relativity (mr) 162.26 g/mol, and the binding energy of allicin on SUR1, Complex 1 and PPARγ are respectively-4.0; -3.0; and-4.1 kcal/mol. The type of interactionbetween allicin and receptors is van der waals. Conclusion:Allicin has good....
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