Palmitoylethanolamide, a naturally occurring lipid, is an orally effective intestinal anti-inflammatory agent

Francesca Borrelli; Barbara Romano; Stefania Petrosino; Ester Pagano; Raffaele Capasso; Diana Coppola; Giovanni Battista; Pierangelo Orlando; Vincenzo Di Marzo; Angelo A Izzo

doi:10.1111/bph.12907

Palmitoylethanolamide, a naturally occurring lipid, is an orally effective intestinal anti-inflammatory agent

Br J Pharmacol. 2015 Jan;172(1):142-58. doi: 10.1111/bph.12907. Epub 2014 Dec 1.

Authors

Francesca Borrelli¹, Barbara Romano, Stefania Petrosino, Ester Pagano, Raffaele Capasso, Diana Coppola, Giovanni Battista, Pierangelo Orlando, Vincenzo Di Marzo, Angelo A Izzo

Affiliation

¹ Department of Pharmacy, University of Naples Federico II, Naples, Italy.

Abstract

Background and purpose: Palmitoylethanolamide (PEA) acts via several targets, including cannabinoid CB1 and CB2 receptors, transient receptor potential vanilloid type-1 (TRPV1) ion channels, peroxisome proliferator-activated receptor alpha (PPAR α) and orphan G protein-coupled receptor 55 (GRR55), all involved in the control of intestinal inflammation. Here, we investigated the effect of PEA in a murine model of colitis.

Experimental approach: Colitis was induced in mice by intracolonic administration of dinitrobenzenesulfonic acid (DNBS). Inflammation was assessed by evaluating inflammatory markers/parameters and by histology; intestinal permeability by a fluorescent method; colonic cell proliferation by immunohistochemistry; PEA and endocannabinoid levels by liquid chromatography mass spectrometry; receptor and enzyme mRNA expression by quantitative RT-PCR.

Key results: DNBS administration caused inflammatory damage, increased colonic levels of PEA and endocannabinoids, down-regulation of mRNA for TRPV1 and GPR55 but no changes in mRNA for CB1 , CB2 and PPARα. Exogenous PEA (i.p. and/or p.o., 1 mg·kg(-1) ) attenuated inflammation and intestinal permeability, stimulated colonic cell proliferation, and increased colonic TRPV1 and CB1 receptor expression. The anti-inflammatory effect of PEA was attenuated or abolished by CB2 receptor, GPR55 or PPARα antagonists and further increased by the TRPV1 antagonist capsazepine.

Conclusions and implications: PEA improves murine experimental colitis, the effect being mediated by CB2 receptors, GPR55 and PPARα, and modulated by TRPV1 channels.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Oral
Amides
Animals
Anti-Inflammatory Agents / administration & dosage
Anti-Inflammatory Agents / pharmacokinetics
Anti-Inflammatory Agents / pharmacology
Anti-Inflammatory Agents / therapeutic use*
Benzenesulfonates
Capsaicin / analogs & derivatives
Capsaicin / pharmacology
Colitis / chemically induced
Colitis / drug therapy*
Colitis / metabolism
Colitis / pathology
Colon / drug effects
Colon / metabolism
Colon / pathology
Disease Models, Animal
Endocannabinoids / metabolism
Ethanolamines / administration & dosage
Ethanolamines / pharmacokinetics
Ethanolamines / pharmacology
Ethanolamines / therapeutic use*
Intestinal Absorption / drug effects
Male
Mice, Inbred ICR
Oleic Acids / metabolism
PPAR alpha / genetics
Palmitic Acids / administration & dosage
Palmitic Acids / pharmacokinetics
Palmitic Acids / pharmacology
Palmitic Acids / therapeutic use*
Peroxidase / metabolism
RNA, Messenger / metabolism
Receptor, Cannabinoid, CB1 / genetics
Receptor, Cannabinoid, CB2 / antagonists & inhibitors
Receptor, Cannabinoid, CB2 / genetics
Receptors, Cannabinoid / genetics
TRPV Cation Channels / antagonists & inhibitors
TRPV Cation Channels / genetics

Substances

Amides
Anti-Inflammatory Agents
Benzenesulfonates
Endocannabinoids
Ethanolamines
GPR55 protein, mouse
Oleic Acids
Oleylethanolamide
PPAR alpha
Palmitic Acids
RNA, Messenger
Receptor, Cannabinoid, CB1
Receptor, Cannabinoid, CB2
Receptors, Cannabinoid
TRPV Cation Channels
TRPV1 protein, mouse
dinitrobenzenesulfonic acid
palmidrol
Peroxidase
capsazepine
Capsaicin