| Literature DB >> 26974385 |
Alessandra Ammazzalorso1, Antonio Carrieri2, Fabio Verginelli3, Isabella Bruno4, Giuseppe Carbonara2, Alessandra D'Angelo4, Barbara De Filippis4, Marialuigia Fantacuzzi4, Rosalba Florio3, Giuseppe Fracchiolla2, Letizia Giampietro4, Antonella Giancristofaro4, Cristina Maccallini4, Alessandro Cama3, Rosa Amoroso5.
Abstract
Recent evidences suggest a moderate activation of Peroxisome Proliferator-Activated Receptors (PPARs) could be favorable in metabolic diseases, reducing side effects given from full agonists. PPAR partial agonists and antagonists represent, to date, interesting tools to better elucidate biological processes modulated by these receptors. In this work are reported new benzenesulfonimide compounds able to block PPARα, synthesized and tested by transactivation assays and gene expression analysis. Some of these compounds showed a dose-dependent antagonistic behavior on PPARα, submicromolar potency, different profiles of selectivity versus PPARγ, and a repressive effect on CPT1A expression. Dockings and molecular dynamics on properly selected benzenesulfonimide derivatives furnished fresh insights into the molecular determinant most likely responsible for PPARα antagonism.Entities:
Keywords: Benzenesulfonimides; CPT1A; Docking; Fibrates; Molecular dynamic; PPAR antagonist; PPARs; Transactivation assay
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Year: 2016 PMID: 26974385 DOI: 10.1016/j.ejmech.2016.02.064
Source DB: PubMed Journal: Eur J Med Chem ISSN: 0223-5234 Impact factor: 6.514