Experimental colitis: decreased Octn2 and Atb0+ expression in rat colonocytes induces carnitine depletion that is reversible by carnitine-loaded liposomes

Giuseppe D'Argenio; Menotti Calvani; Amelia Casamassimi; Orsolina Petillo; Sabrina Margarucci; Monica Rienzo; Ivana Peluso; Riccardo Calvani; Alfredo Ciccodicola; Nicola Caporaso; Gianfranco Peluso

doi:10.1096/fj.06-5950fje

Experimental colitis: decreased Octn2 and Atb0+ expression in rat colonocytes induces carnitine depletion that is reversible by carnitine-loaded liposomes

FASEB J. 2006 Dec;20(14):2544-6. doi: 10.1096/fj.06-5950fje. Epub 2006 Oct 25.

Authors

Giuseppe D'Argenio¹, Menotti Calvani, Amelia Casamassimi, Orsolina Petillo, Sabrina Margarucci, Monica Rienzo, Ivana Peluso, Riccardo Calvani, Alfredo Ciccodicola, Nicola Caporaso, Gianfranco Peluso

Affiliation

¹ Gastroenterology Unit, Department of Clinical and Experimental Medicine, University Federico II, Naples, Italy.

PMID: 17065219
DOI: 10.1096/fj.06-5950fje

Abstract

Carnitine transporters have recently been implicated in susceptibility to inflammatory bowel disease (IBD). Because carnitine is required for beta-oxidation, it was suggested that decreased carnitine transporters, and hence reduced carnitine uptake, could lead to impaired fatty acid oxidation in intestinal epithelial cells, and to cell injury. We investigated this issue by examining the expression of the carnitine transporters OCTN2 and ATB0+, and butyrate metabolism in colonocytes in a rat model of IBD induced by trinitrobenzene sulfonic acid (TNBS). We found that Octn2 and Atb0+ expression was decreased in inflammatory samples at translational and functional level. Butyrate oxidation, evaluated based on CO2 production and acetyl-coenzyme A synthesis, was deranged in colonocytes from TNBS-treated rats. Treatment with carnitine-loaded liposomes corrected the butyrate metabolic alterations in vitro and reduced the severity of colitis in vivo. These results suggest that carnitine depletion in colonocytes is associated with the inability of mitochondria to maintain normal butyrate beta-oxidation. Our data indicate that carnitine is a rate-limiting factor for the maintenance of physiological butyrate oxidation in colonic cells. This hypothesis could also explain the contradictory therapeutic efficacy of butyrate supplementation observed in clinical trials of IBD.

MeSH terms

Amino Acid Sequence
Amino Acid Transport System ASC / metabolism*
Animals
Base Sequence
Butyric Acid / metabolism
Carnitine / metabolism*
Colitis / chemically induced
Colitis / metabolism*
Liposomes / chemistry
Liposomes / metabolism
Molecular Sequence Data
Neurotransmitter Transport Proteins / chemistry
Neurotransmitter Transport Proteins / genetics
Neurotransmitter Transport Proteins / metabolism*
Organic Cation Transport Proteins / genetics
Organic Cation Transport Proteins / metabolism*
Rats
Rats, Wistar
Solute Carrier Family 22 Member 5
Trinitrobenzenesulfonic Acid / toxicity

Substances

Amino Acid Transport System ASC
Liposomes
Neurotransmitter Transport Proteins
Organic Cation Transport Proteins
Slc22a5 protein, rat
Slc6a14 protein, rat
Solute Carrier Family 22 Member 5
Butyric Acid
Trinitrobenzenesulfonic Acid
Carnitine

Abstract

MeSH terms

Substances

Grants and funding