PPAR gamma targeted molecular docking and synthesis of some new amide and urea substituted 1, 3, 4-thiadiazole derivative as antidiabetic compound |
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Authors: | Yogesh Vaishnav Dhansay Dewangan Shekhar Verma Achal Mishra Alok Singh Thakur Pranita Kashyap Santosh Kumar Verma |
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Affiliation: | 1. Shri Shankaracharya Technical Campus, Shri Shankaracharya Group of Institutions, Bhilai, India;2. Department of Pharmaceutical Chemistry, Shri Rawatpura Sarkar Institute of Pharmacy, Kumhari, India;3. Department of Pharmaceutical Chemistry, Dr. R.G. Bhoyar Institute of Pharmaceutical Education and Research, Wardha, India;4. School of Chemistry and Chemical Engineering, Yulin University, Yulin, P.R. China |
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Abstract: | The PPAR-γ agonist enhances the insulin sensitivity and avoids the disorganized hyperglycemic by promoting the insulin guided cellular uptake of blood glucose. Therefore, in the present work PPAR-γ has chosen as the target for the molecular docking study to design an effective agonist of the same. By this research work an effort has been made to prepare amide and urea series of 1, 3, 4-thiadiazole derivatives as 4-substituted-N-(5-(4-(1-piperidino)1-piperidinyl)-1,3,4-(2-thiadiazolyl)benzamide (4a-f) and 1-(4-substitutedphenyl)-3-(5-(4-(1-piperidino)1-piperidinyl)-1,3,4-(2-thiadiazolyl)urea (6a-f) . Both the docking score as well as the pharmacological animal study data has been suggested that the electron donating group containing compound 4f and 6f are most potent molecules for the antidiabetic activity close to the standard drug pioglitazone. It was further observed that the unsubstituted aromatic ring containing derivatives have also considerable effect (4a and 6a) than the electron withdrawing containing derivatives. After the comparison of biological data for amide and urea series, it was concluded that the urea (6a-f) series is more effective than the amide series. |
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