Design, development and evaluation of novel dual PPARδ/PPARγ agonists

Design, development and evaluation of novel dual PPARδ/PPARγ agonists

Type 2 diabetes is at epidemic proportions and thus development of novel pharmaceutical therapies for improving insulin sensitivity has become of paramount importance. The objectives of the current study were to develop novel dual PPARγ/δ agonists without the deleterious side effects associated with...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2013-02, Vol.23 (3), p.873-879
Hauptverfasser: Gathiaka, Symon, Nanayakkara, Gayani, Boncher, Tracey, Acevedo, Orlando, Wyble, Johnathon, Patel, Sagar, Patel, Akash, Shane, Mary Elizabeth, Bonkowski, Blake, Wieczorek, Jason, Rong, Yinghui, Huggins, Kevin, Smith, Forest, Amin, Rajesh H.
Format: Artikel
Sprache:eng
Schlagworte:
Adiposity
AutoDock vina
Diabetes
Dose-Response Relationship, Drug
Drug Combinations
Drug Design
Hypoglycemic Agents - chemical synthesis
Hypoglycemic Agents - chemistry
Hypoglycemic Agents - pharmacology
Models, Molecular
Molecular Docking Simulation
Molecular Structure
Peroxisomal proliferator activating receptor (PPAR)
PPAR delta - agonists
PPAR gamma - agonists
Protein Binding - drug effects
Transciptional activity
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Zusammenfassung:Type 2 diabetes is at epidemic proportions and thus development of novel pharmaceutical therapies for improving insulin sensitivity has become of paramount importance. The objectives of the current study were to develop novel dual PPARγ/δ agonists without the deleterious side effects associated with full PPARγ agonists. Docking simulations of 23 novel compounds within the ligand binding domain of PPARγ/δ were performed using AutoDock Vina which consistently reproduced experimental binding poses from known PPAR agonists. Comparisons were made and described with other docking programs AutoDock and Surflex-Dock (from SYBYL-X). Biological evaluation of compounds was accomplished by transcriptional promoter activity assays, quantitative PCR gene analysis for known PPARγ/δ targets as well as in vitro assays for lipid accumulation and mitochondrial biogenesis verses known PPAR agonists. We found one (compound 9) out of the 23 compounds evaluated, to be the most potent and selective dual PPARγ/δ agonist which did not display the deleterious side effects associated with full PPARγ agonists. Type 2 diabetes is at epidemic proportions and thus development of novel pharmaceutical therapies for improving insulin sensitivity has become of paramount importance. The objectives of the current study were to develop novel dual PPARγ/δ agonists without the deleterious side effects associated with full PPARγ agonists. Docking simulations of 23 novel compounds within the ligand binding domain of PPARγ/δ were performed using AutoDock Vina which consistently reproduced experimental binding poses from known PPAR agonists. Comparisons were made and described with other docking programs AutoDock and Surflex-Dock (from SYBYL-X). Biological evaluation of compounds was accomplished by transcriptional promoter activity assays, quantitative PCR gene analysis for known PPARγ/δ targets as well as in vitro assays for lipid accumulation and mitochondrial biogenesis verses known PPAR agonists. We found one (compound 9) out of the 23 compounds evaluated, to be the most potent and selective dual PPARγ/δ agonist which did not display the deleterious side effects associated with full PPARγ agonists.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2012.11.060