An anorexic lipid mediator regulated by feeding
- F. Rodríguez De Fonsecab, e(Author),
- M. Navarrob(Author),
- R. Gómezb(Author),
- L. Escuredob(Author),
- F. Navad(Author),
- J. Fuf(Author)
- aUniversidad Nacional Autónoma de México,
- bComplutense University,
- cUniversity of California at Irvine,
- dUniversity of Cagliari,
- eHospital Regional Universitario Carlos Haya,
- fDepartment of Pharmacology
Open access
Publication Information
Output type
Original language
EnglishPages from-to (Number of pages)
Pages 209-212 (4 pages)Journal (Volume, Issue Number)
Nature (Volume 414, Issue 6860)Publication milestones
- Published - 08/11/2001
Publication status
ISSN
0028-0836External Publication IDs
- Scopus: 0035829625
- PubMed: 11700558
Abstract
Oleylethanolamide (OEA) is a natural analogue of the endogenous cannabinoid anandamide. Like anandamide, OEA is produced in cells in a stimulus-dependent manner and is rapidly eliminated by enzymatic hydrolysis, suggesting a function in cellular signalling 1. However, OEA does not activate cannabinoid receptors and its biological functions are still unknown 2. Here we show that, in rats, food deprivation markedly reduces OEA biosynthesis in the small intestine. Administration of OEA causes a potent and persistent decrease in food intake and gain in body mass. This anorexic effect is behaviourally selective and is associated with the discrete activation of brain regions (the paraventricular hypothalamic nucleus and the nucleus of the solitary tract) involved in the control of satiety. OEA does not affect food intake when injected into the brain ventricles, and its anorexic actions are prevented when peripheral sensory fibres are removed by treatment with capsaicin. These results indicate that OEA is a lipid mediator involved in the peripheral regulation of feeding.