PLoS ONE (Jan 2013)

Fatty acid transporter CD36 mediates hypothalamic effect of fatty acids on food intake in rats.

  • Valentine S Moullé,
  • Christelle Le Foll,
  • Erwann Philippe,
  • Nadim Kassis,
  • Claude Rouch,
  • Nicolas Marsollier,
  • Linh-Chi Bui,
  • Christophe Guissard,
  • Julien Dairou,
  • Anne Lorsignol,
  • Luc Pénicaud,
  • Barry E Levin,
  • Céline Cruciani-Guglielmacci,
  • Christophe Magnan

DOI
https://doi.org/10.1371/journal.pone.0074021
Journal volume & issue
Vol. 8, no. 9
p. e74021

Abstract

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Variations in plasma fatty acid (FA) concentrations are detected by FA sensing neurons in specific brain areas such as the hypothalamus. These neurons play a physiological role in the control of food intake and the regulation of hepatic glucose production. Le Foll et al. previously showed in vitro that at least 50% of the FA sensing in ventromedial hypothalamic (VMH) neurons is attributable to the interaction of long chain FA with FA translocase/CD36 (CD36). The present work assessed whether in vivo effects of hypothalamic FA sensing might be partly mediated by CD36 or intracellular events such as acylCoA synthesis or β-oxidation. To that end, a catheter was implanted in the carotid artery toward the brain in male Wistar rats. After 1 wk recovery, animals were food-deprived for 5 h, then 10 min infusions of triglyceride emulsion, Intralipid +/- heparin (IL, IL(H), respectively) or saline/heparin (SH) were carried out and food intake was assessed over the next 5 h. Experimental groups included: 1) Rats previously injected in ventromedian nucleus (VMN) with shRNA against CD36 or scrambled RNA; 2) Etomoxir (CPT1 inhibitor) or saline co-infused with IL(H)/S(H); and 3) Triacsin C (acylCoA synthase inhibitor) or saline co-infused with IL(H)/S(H). IL(H) significantly lowered food intake during refeeding compared to S(H) (p<0.001). Five hours after refeeding, etomoxir did not affect this inhibitory effect of IL(H) on food intake while VMN CD36 depletion totally prevented it. Triacsin C also prevented IL(H) effects on food intake. In conclusion, the effect of FA to inhibit food intake is dependent on VMN CD36 and acylCoA synthesis but does not required FA oxidation.