Metabolic and psychiatric effects of acyl coenzyme A binding protein (ACBP)/diazepam binding inhibitor (DBI)

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作者
Adrien Joseph
Stéphanie Moriceau
Valentina Sica
Gerasimos Anagnostopoulos
Jonathan Pol
Isabelle Martins
Antoine Lafarge
Maria Chiara Maiuri
Marion Leboyer
Josephine Loftus
Frank Bellivier
Raoul Belzeaux
Fabrice Berna
Bruno Etain
Delphine Capdevielle
Philippe Courtet
Caroline Dubertret
Julien Dubreucq
D’. Amato Thierry
Guillaume Fond
Sebastien Gard
Pierre-Michel Llorca
Jasmina Mallet
David Misdrahi
Emilie Olié
Christine Passerieux
Mircea Polosan
Paul Roux
Ludovic Samalin
Franck Schürhoff
Raymond Schwan
Christophe Magnan
Franck Oury
José M. Bravo-San Pedro
Guido Kroemer
机构
[1] Université de Paris,Centre de Recherche des Cordeliers, Equipe labellisée par la Ligue Contre le Cancer
[2] Sorbonne Université,Metabolomics and Cell Biology Platforms
[3] Inserm U1138,Faculté de Médecine
[4] Institut Gustave Roussy,Cell Biology Group, Department of Experimental and Health Sciences
[5] Université de Paris Saclay,AP
[6] INSERM U1151,HP, HU Henri Mondor, Departement Medico
[7] Institut Necker Enfants-Malades (INEM),Universitaire de Psychiatrie et d’Addictologie (DMU ADAPT)
[8] Université Paris Descartes-Sorbonne-Paris Cité,Pôle de Psychiatrie
[9] Pompeu Fabra University (UPF),AP
[10] Gustave Roussy Comprehensive Cancer Institute,HP, GH Saint
[11] Fondation FondaMental,Louis—Lariboisière—Fernand Widal, Pôle Neurosciences Tête et Cou, INSERM UMRS 1144
[12] Université Paris Est Créteil,Hôpitaux Universitaires de Strasbourg
[13] Inserm U955,Service Universitaire de Psychiatrie Adulte, Hôpital la Colombière, CHRU Montpellier
[14] IMRB,Department of Emergency Psychiatry and Acute Care
[15] Laboratoire Neuro-Psychiatrie translationnelle,AP
[16] Federation Hospitalo-Universitaire de Médecine de Precision (FHU IMPACT),HP, Groupe Hospitalo
[17] Fondation FondaMental Créteil,Universitaire Nord, DMU ESPRIT, Service de Psychiatrie et Addictologie. Hopital Louis Mourier, Colombes, Inserm U1266, Faculté de Médecine
[18] Centre Hospitalier Princesse Grace,INSERM U1028, CNRS UMR5292, Centre de Recherche en Neurosciences de Lyon
[19] University Paris Diderot,Centre Expert Troubles Bipolaires
[20] Pôle de Psychiatrie,CHU Clermont
[21] Assistance Publique Hôpitaux de Marseille,Ferrand, Department of Psychiatry
[22] INT-UMR7289,Service Universitaire de Psychiatrie d’Adultes, Centre Hospitalier de Versailles, Le Chesnay
[23] CNRS Aix-Marseille Université,Suzhou Institute for Systems Medicine
[24] Université de Strasbourg,Karolinska Institute, Department of Women’s and Children’s Health
[25] INSERM U1114,undefined
[26] Fédération de Médecine Translationnelle de Strasbourg,undefined
[27] Université Montpellier 1,undefined
[28] Inserm 1061,undefined
[29] Lapeyronie Hospital,undefined
[30] CHU Montpellier,undefined
[31] PSNREC,undefined
[32] Univ Montpellier,undefined
[33] INSERM,undefined
[34] CHU Montpellier,undefined
[35] Université de Paris,undefined
[36] Centre Référent de Réhabilitation Psychosociale et de Remédiation Cognitive (C3R),undefined
[37] CH,undefined
[38] Université Claude Bernard Lyon 1,undefined
[39] Equipe PSYR2,undefined
[40] Centre Hospitalier Le Vinatier,undefined
[41] Pole Est,undefined
[42] AP-HM,undefined
[43] Aix-Marseille University,undefined
[44] School of Medicine—La Timone Medical Campus,undefined
[45] EA 3279,undefined
[46] EReSS—Health Service Research and Quality of Life Center,undefined
[47] Service de Psychiatrie Adulte,undefined
[48] Hôpital Charles-Perrens,undefined
[49] University of Clermont Auvergne,undefined
[50] Université Paris-Saclay,undefined
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摘要
Acyl coenzyme A binding protein (ACBP), also known as diazepam binding inhibitor (DBI) is a multifunctional protein with an intracellular action (as ACBP), as well as with an extracellular role (as DBI). The plasma levels of soluble ACBP/DBI are elevated in human obesity and reduced in anorexia nervosa. Accumulating evidence indicates that genetic or antibody-mediated neutralization of ACBP/DBI has anorexigenic effects, thus inhibiting food intake and inducing lipo-catabolic reactions in mice. A number of anorexiants have been withdrawn from clinical development because of their side effects including an increase in depression and suicide. For this reason, we investigated the psychiatric impact of ACBP/DBI in mouse models and patient cohorts. Intravenously (i.v.) injected ACBP/DBI protein conserved its orexigenic function when the protein was mutated to abolish acyl coenzyme A binding, but lost its appetite-stimulatory effect in mice bearing a mutation in the γ2 subunit of the γ-aminobutyric acid (GABA) A receptor (GABAAR). ACBP/DBI neutralization by intraperitoneal (i.p.) injection of a specific mAb blunted excessive food intake in starved and leptin-deficient mice, but not in ghrelin-treated animals. Neither i.v. nor i.p. injected anti-ACBP/DBI antibody affected the behavior of mice in the dark–light box and open-field test. In contrast, ACBP/DBI increased immobility in the forced swim test, while anti-ACBP/DBI antibody counteracted this sign of depression. In patients diagnosed with therapy-resistant bipolar disorder or schizophrenia, ACBP/DBI similarly correlated with body mass index (BMI), not with the psychiatric diagnosis. Patients with high levels of ACBP/DBI were at risk of dyslipidemia and this effect was independent from BMI, as indicated by multivariate analysis. In summary, it appears that ACBP/DBI neutralization has no negative impact on mood and that human depression is not associated with alterations in ACBP/DBI concentrations.
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