Integrative study of diet-induced mouse models of NAFLD identifies PPARα as a sexually dimorphic drug target

Sarra Smati; Arnaud Polizzi; Anne Fougerat; Sandrine Ellero-Simatos; Yuna Blum; Yannick Lippi; Marion Régnier; Alexia Laroyenne; Marine Huillet; Muhammad Arif; Cheng Zhang; Frederic Lasserre; Alain Marrot; Talal Al Saati; JingHong Wan; Caroline Sommer; Claire Naylies; Aurelie Batut; Celine Lukowicz; Tiffany Fougeray; Blandine Tramunt; Patricia Dubot; Lorraine Smith; Justine Bertrand-Michel; Nathalie Hennuyer; Jean-Philippe Pradere; Bart Staels; Remy Burcelin; Françoise Lenfant; Jean-François Arnal; Thierry Levade; Laurence Gamet-Payrastre; Sandrine Lagarrigue; Nicolas Loiseau; Sophie Lotersztajn; Catherine Postic; Walter Wahli; Christophe Bureau; Maeva Guillaume; Adil Mardinoglu; Alexandra Montagner; Pierre Gourdy; Hervé Guillou

doi:10.1136/gutjnl-2020-323323

Integrative study of diet-induced mouse models of NAFLD identifies PPARα as a sexually dimorphic drug target

Gut. 2022 Apr;71(4):807-821. doi: 10.1136/gutjnl-2020-323323. Epub 2021 Apr 26.

Authors

Sarra Smati^{1

2}, Arnaud Polizzi¹, Anne Fougerat¹, Sandrine Ellero-Simatos¹, Yuna Blum^{3

4}, Yannick Lippi¹, Marion Régnier¹, Alexia Laroyenne¹, Marine Huillet¹, Muhammad Arif⁵, Cheng Zhang⁵, Frederic Lasserre¹, Alain Marrot¹, Talal Al Saati⁶, JingHong Wan^{7

8}, Caroline Sommer¹, Claire Naylies¹, Aurelie Batut², Celine Lukowicz¹, Tiffany Fougeray¹, Blandine Tramunt², Patricia Dubot^{9

10}, Lorraine Smith¹, Justine Bertrand-Michel², Nathalie Hennuyer¹¹, Jean-Philippe Pradere², Bart Staels¹¹, Remy Burcelin², Françoise Lenfant², Jean-François Arnal², Thierry Levade^{9

10}, Laurence Gamet-Payrastre¹, Sandrine Lagarrigue¹², Nicolas Loiseau¹, Sophie Lotersztajn^{7

8}, Catherine Postic¹³, Walter Wahli^{1

14

15}, Christophe Bureau¹⁶, Maeva Guillaume¹⁶, Adil Mardinoglu^{5

17}, Alexandra Montagner², Pierre Gourdy^#^{18

19}, Hervé Guillou^#²⁰

Affiliations

¹ Toxalim (Research Center in Food Toxicology), INRAE, ENVT, INP- PURPAN, UMR 1331, UPS, Université de Toulouse, Toulouse, France.
² Institut des Maladies Métaboliques et Cardiovasculaires (I2MC), UMR1297, INSERM/UPS, Université de Toulouse, Toulouse, France.
³ CIT, Ligue Nationale Contre Le Cancer, Paris, France.
⁴ IGDR UMR 6290, CNRS, Université de Rennes 1, Rennes, France.
⁵ Science for Life Laboratory, KTH-Royal Institute of Technology, Solna, Sweden.
⁶ Experimental Histopathology Department, INSERM US006-CREFRE, University Hospital of Toulouse, Toulouse, France.
⁷ INSERM-UMR1149, Centre de Recherche sur l'Inflammation, Paris, France.
⁸ Sorbonne Paris Cité, Laboratoire d'Excellence Inflamex, Faculté de Médecine, Site Xavier Bichat, Université Paris Diderot, Paris, France.
⁹ Laboratoire de Biochimie Métabolique, CHU Toulouse, Toulouse, France.
¹⁰ INSERM U1037, CRCT, Université Paul Sabatier, Toulouse, France.
¹¹ Univ. Lille, INSERM, CHU Lille, Institut Pasteur de Lille, U1011-EGID, F-59000, Lille, France.
¹² INRAE, INSTITUT AGRO, PEGASE UMR1348, 35590, Saint-Gilles, France.
¹³ Université de Paris, Institut Cochin, CNRS, INSERM, Paris, France.
¹⁴ Lee Kong Chian School of Medicine, Nanyang Technological University, Singapore.
¹⁵ Center for Integrative Genomics, University of Lausanne, Le Génopode, Lausanne, Switzerland.
¹⁶ Hepatology Unit, Rangueil Hospital Toulouse, Paul Sabatier University Toulouse 3, Toulouse, France.
¹⁷ Centre for Host-Microbiome Interactions, Faculty of Dentistry, Oral & Craniofacial Sciences, King's College London, London, UK.
¹⁸ Institut des Maladies Métaboliques et Cardiovasculaires (I2MC), UMR1297, INSERM/UPS, Université de Toulouse, Toulouse, France herve.guillou@inrae.fr pierre.gourdy@inserm.fr.
¹⁹ Endocrinology-Diabetology-Nutrition Department, Toulouse University Hospital, Toulouse, France.
²⁰ Toxalim (Research Center in Food Toxicology), INRAE, ENVT, INP- PURPAN, UMR 1331, UPS, Université de Toulouse, Toulouse, France herve.guillou@inrae.fr pierre.gourdy@inserm.fr.

^# Contributed equally.

PMID: 33903148
DOI: 10.1136/gutjnl-2020-323323

Abstract

Objective: We evaluated the influence of sex on the pathophysiology of non-alcoholic fatty liver disease (NAFLD). We investigated diet-induced phenotypic responses to define sex-specific regulation between healthy liver and NAFLD to identify influential pathways in different preclinical murine models and their relevance in humans.

Design: Different models of diet-induced NAFLD (high-fat diet, choline-deficient high-fat diet, Western diet or Western diet supplemented with fructose and glucose in drinking water) were compared with a control diet in male and female mice. We performed metabolic phenotyping, including plasma biochemistry and liver histology, untargeted large-scale approaches (liver metabolome, lipidome and transcriptome), gene expression profiling and network analysis to identify sex-specific pathways in the mouse liver.

Results: The different diets induced sex-specific responses that illustrated an increased susceptibility to NAFLD in male mice. The most severe lipid accumulation and inflammation/fibrosis occurred in males receiving the high-fat diet and Western diet, respectively. Sex-biased hepatic gene signatures were identified for these different dietary challenges. The peroxisome proliferator-activated receptor α (PPARα) co-expression network was identified as sexually dimorphic, and in vivo experiments in mice demonstrated that hepatocyte PPARα determines a sex-specific response to fasting and treatment with pemafibrate, a selective PPARα agonist. Liver molecular signatures in humans also provided evidence of sexually dimorphic gene expression profiles and the sex-specific co-expression network for PPARα.

Conclusions: These findings underscore the sex specificity of NAFLD pathophysiology in preclinical studies and identify PPARα as a pivotal, sexually dimorphic, pharmacological target.

Trial registration number: NCT02390232.

Keywords: gene expression; lipid metabolism; liver metabolism; nonalcoholic steatohepatitis.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Diet, High-Fat / adverse effects
Disease Models, Animal
Female
Humans
Lipid Metabolism
Liver / metabolism
Male
Mice
Mice, Inbred C57BL
Non-alcoholic Fatty Liver Disease* / metabolism
PPAR alpha / metabolism

Substances

PPAR alpha

Associated data

ClinicalTrials.gov/NCT02390232