Identificador persistente para citar o vincular este elemento: http://hdl.handle.net/10662/19858
Títulos: Acyl-CoA-Binding protein is a lipogenic factor that triggers food intake and obesity
Autores/as: Bravo San Pedro, José Manuel
Sica, Valentina
Martins, Isabelle
Pol, Jonathan
Loos, Friedemann
Maiuri, Maria Chiara
Durand, Sylvere
Bossut, Noélie
Anagnostopoulos, Gerasimos
Niso Santano, Mireia
Drake Aranda, Fernando
Ramirez Pardo, Ignacio
Denom, Justine
Boedec, Erwan
Gorwood, Philip
Ramoz, Nicolas
Clément, Karine
Pelloux, Veronique
Rohia, Alili
Pattou, François
Raverdy, Violeta
Caiazzo, Robert
Denis, Raphaël G.P.
Boya, Patricia
Galluzzi, Lorenzo
Madeo, Frank
Migrenne Li, Stéphanie
Cruciani Guglielmacci, Céline
Tavernarakis, Nektarios
López Otín, Carlos
Magnan, Christophe
Kroemer, Guido
Palabras clave: Anorexia;Anorexy;Autofagia;Autophagy;Obesidad;Obesity;Lipid metabolism;Metabolismo de los lípidos
Fecha de publicación: 2019
Editor/a: Sciendirect
Resumen: Autophagy facilitates the adaptation to nutritional stress. Here, we show that short-term starvation of cultured cells or mice caused the autophagy-dependent cellular release of acyl-CoA-binding protein (ACBP, also known as diazepam-binding inhibitor, DBI) and consequent ACBP-mediated feedback inhibition of autophagy. Importantly, ACBP levels were elevated in obese patients and reduced in anorexia nervosa. In mice, systemic injection of ACBP protein inhibited autophagy, induced lipogenesis, reduced glycemia, and stimulated appetite as well as weight gain. We designed three approaches to neutralize ACBP, namely, inducible whole-body knockout, systemic administration of neutralizing antibodies, and induction of antiACBP autoantibodies in mice. ACBP neutralization enhanced autophagy, stimulated fatty acid oxidation, inhibited appetite, reduced weight gain in the context of a high-fat diet or leptin deficiency, and accelerated weight loss in response to dietary changes. In conclusion, neutralization of ACBP might constitute a strategy for treating obesity and its co-morbidities.
URI: http://hdl.handle.net/10662/19858
DOI: 10.1016/j.cmet.2019.07.010
Colección:DBYBM - Artículos

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