Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines

To further understand the pharmacological properties of N-oleoylethanolamine (OEA), a naturally occurring lipid that activates peroxisome proliferator-activated receptor alpha (PPARα), we designed sulfamoyl analogs based on its structure. Among the compounds tested, N-octadecyl-N′-propylsulfamide (C...

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Autores principales: Moreno-Santos, Inmaculada, Pavón, Francisco Javier, Romero-Cuevas, Miguel, Serrano, Antonia, Cano, Carolina, Suardíaz, Margarita, Decara, Juan, Suarez, Juan, de Fonseca, Fernando Rodríguez, Macías-González, Manuel
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961330/
https://www.ncbi.nlm.nih.gov/pubmed/24651609
http://dx.doi.org/10.1371/journal.pone.0092195
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author Moreno-Santos, Inmaculada
Pavón, Francisco Javier
Romero-Cuevas, Miguel
Serrano, Antonia
Cano, Carolina
Suardíaz, Margarita
Decara, Juan
Suarez, Juan
de Fonseca, Fernando Rodríguez
Macías-González, Manuel
author_facet Moreno-Santos, Inmaculada
Pavón, Francisco Javier
Romero-Cuevas, Miguel
Serrano, Antonia
Cano, Carolina
Suardíaz, Margarita
Decara, Juan
Suarez, Juan
de Fonseca, Fernando Rodríguez
Macías-González, Manuel
author_sort Moreno-Santos, Inmaculada
collection PubMed
description To further understand the pharmacological properties of N-oleoylethanolamine (OEA), a naturally occurring lipid that activates peroxisome proliferator-activated receptor alpha (PPARα), we designed sulfamoyl analogs based on its structure. Among the compounds tested, N-octadecyl-N′-propylsulfamide (CC7) was selected for functional comparison with OEA. The performed studies include the following computational and biological approaches: 1) molecular docking analyses; 2) molecular biology studies with PPARα; 3) pharmacological studies on feeding behavior and visceral analgesia. For the docking studies, we compared OEA and CC7 data with crystallization data obtained with the reference PPARα agonist GW409544. OEA and CC7 interacted with the ligand-binding domain of PPARα in a similar manner to GW409544. Both compounds produced similar transcriptional activation by in vitro assays, including the GST pull-down assay and reporter gene analysis. In addition, CC7 and OEA induced the mRNA expression of CPT1a in HpeG2 cells through PPARα and the induction was avoided with PPARα-specific siRNA. In vivo studies in rats showed that OEA and CC7 had anorectic and antiobesity activity and induced both lipopenia and decreases in hepatic fat content. However, different effects were observed when measuring visceral pain; OEA produced visceral analgesia whereas CC7 showed no effects. These results suggest that OEA activity on the PPARα receptor (e.g., lipid metabolism and feeding behavior) may be dissociated from other actions at alternative targets (e.g., pain) because other non cannabimimetic ligands that interact with PPARα, such as CC7, do not reproduce the full spectrum of the pharmacological activity of OEA. These results provide new opportunities for the development of specific PPARα-activating drugs focused on sulfamide derivatives with a long alkyl chain for the treatment of metabolic dysfunction.
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spelling pubmed-39613302014-03-27 Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines Moreno-Santos, Inmaculada Pavón, Francisco Javier Romero-Cuevas, Miguel Serrano, Antonia Cano, Carolina Suardíaz, Margarita Decara, Juan Suarez, Juan de Fonseca, Fernando Rodríguez Macías-González, Manuel PLoS One Research Article To further understand the pharmacological properties of N-oleoylethanolamine (OEA), a naturally occurring lipid that activates peroxisome proliferator-activated receptor alpha (PPARα), we designed sulfamoyl analogs based on its structure. Among the compounds tested, N-octadecyl-N′-propylsulfamide (CC7) was selected for functional comparison with OEA. The performed studies include the following computational and biological approaches: 1) molecular docking analyses; 2) molecular biology studies with PPARα; 3) pharmacological studies on feeding behavior and visceral analgesia. For the docking studies, we compared OEA and CC7 data with crystallization data obtained with the reference PPARα agonist GW409544. OEA and CC7 interacted with the ligand-binding domain of PPARα in a similar manner to GW409544. Both compounds produced similar transcriptional activation by in vitro assays, including the GST pull-down assay and reporter gene analysis. In addition, CC7 and OEA induced the mRNA expression of CPT1a in HpeG2 cells through PPARα and the induction was avoided with PPARα-specific siRNA. In vivo studies in rats showed that OEA and CC7 had anorectic and antiobesity activity and induced both lipopenia and decreases in hepatic fat content. However, different effects were observed when measuring visceral pain; OEA produced visceral analgesia whereas CC7 showed no effects. These results suggest that OEA activity on the PPARα receptor (e.g., lipid metabolism and feeding behavior) may be dissociated from other actions at alternative targets (e.g., pain) because other non cannabimimetic ligands that interact with PPARα, such as CC7, do not reproduce the full spectrum of the pharmacological activity of OEA. These results provide new opportunities for the development of specific PPARα-activating drugs focused on sulfamide derivatives with a long alkyl chain for the treatment of metabolic dysfunction. Public Library of Science 2014-03-20 /pmc/articles/PMC3961330/ /pubmed/24651609 http://dx.doi.org/10.1371/journal.pone.0092195 Text en © 2014 Moreno-Santos et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Moreno-Santos, Inmaculada
Pavón, Francisco Javier
Romero-Cuevas, Miguel
Serrano, Antonia
Cano, Carolina
Suardíaz, Margarita
Decara, Juan
Suarez, Juan
de Fonseca, Fernando Rodríguez
Macías-González, Manuel
Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title_full Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title_fullStr Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title_full_unstemmed Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title_short Computational and Biological Evaluation of N-octadecyl-N′-propylsulfamide, a Selective PPARα Agonist Structurally Related to N-acylethanolamines
title_sort computational and biological evaluation of n-octadecyl-n′-propylsulfamide, a selective pparα agonist structurally related to n-acylethanolamines
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961330/
https://www.ncbi.nlm.nih.gov/pubmed/24651609
http://dx.doi.org/10.1371/journal.pone.0092195
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