1. CRISPR/Cas9-mediated inactivation of the phosphatase activity of soluble epoxide hydrolase prevents obesity and cardiac ischemic injury
- Author
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Leuillier, Matthieu, Duflot, Thomas, Ménoret, Séverine, Messaoudi, Hind, Djerada, Zoubir, Groussard, Déborah, Denis, Raphaël GP, Chevalier, Laurence, Karoui, Ahmed, Panthu, Baptiste, Thiébaut, Pierre-Alain, Schmitz-Afonso, Isabelle, Nobis, Séverine, Campart, Cynthia, Henry, Tiphaine, Sautreuil, Camille, Luquet, Serge H, Beseme, Olivia, Féliu, Catherine, Peyret, Hélène, Nicol, Lionel, Henry, Jean-Paul, Renet, Sylvanie, Mulder, Paul, Wan, Debin, Tesson, Laurent, Heslan, Jean-Marie, Duché, Angéline, Jacques, Sébastien, Ziegler, Frédéric, Brunel, Valéry, Rautureau, Gilles JP, Monteil, Christelle, do Rego, Jean-Luc, do Rego, Jean-Claude, Afonso, Carlos, Hammock, Bruce, Madec, Anne-Marie, Pinet, Florence, Richard, Vincent, Anegon, Ignacio, Guignabert, Christophe, Morisseau, Christophe, and Bellien, Jérémy
- Subjects
Biochemistry and Cell Biology ,Biomedical and Clinical Sciences ,Biological Sciences ,Nutrition ,Genetics ,Cardiovascular ,Obesity ,2.1 Biological and endogenous factors ,Metabolic and endocrine ,Animals ,Female ,Male ,Rats ,CRISPR-Cas Systems ,Epoxide Hydrolases ,Heart Diseases ,Heart Injuries ,Insulin Resistance ,Lysophospholipids ,Phosphoric Monoester Hydrolases ,Reperfusion Injury ,Soluble epoxide hydrolase ,Lipid phosphatase ,CRISPR-Cas9 ,Thermogenesis ,Cardiac ischemic injury - Abstract
IntroductionAlthough the physiological role of the C-terminal hydrolase domain of the soluble epoxide hydrolase (sEH-H) is well investigated, the function of its N-terminal phosphatase activity (sEH-P) remains unknown.ObjectivesThis study aimed to assess in vivo the physiological role of sEH-P.MethodsCRISPR/Cas9 was used to generate a novel knock-in (KI) rat line lacking the sEH-P activity.ResultsThe sEH-P KI rats has a decreased metabolism of lysophosphatidic acids to monoacyglycerols. KI rats grew almost normally but with less weight and fat mass gain while insulin sensitivity was increased compared to wild-type rats. This lean phenotype was more marked in males than in female KI rats and mainly due to decreased food consumption and enhanced energy expenditure. In fact, sEH-P KI rats had an increased lipolysis allowing to supply fatty acids as fuel to potentiate brown adipose thermogenesis under resting condition and upon cold exposure. The potentiation of thermogenesis was abolished when blocking PPARγ, a nuclear receptor activated by intracellular lysophosphatidic acids, but also when inhibiting simultaneously sEH-H, showing a functional interaction between the two domains. Furthermore, sEH-P KI rats fed a high-fat diet did not gain as much weight as the wild-type rats, did not have increased fat mass and did not develop insulin resistance or hepatic steatosis. In addition, sEH-P KI rats exhibited enhanced basal cardiac mitochondrial activity associated with an enhanced left ventricular contractility and were protected against cardiac ischemia-reperfusion injury.ConclusionOur study reveals that sEH-P is a key player in energy and fat metabolism and contributes together with sEH-H to the regulation of cardiometabolic homeostasis. The development of pharmacological inhibitors of sEH-P appears of crucial importance to evaluate the interest of this promising therapeutic strategy in the management of obesity and cardiac ischemic complications.
- Published
- 2023