Obesogen effects after perinatal exposure of 4,4′-sulfonyldiphenol (Bisphenol S) in C57BL/6 mice

6533b85cfe1ef96bd12bc021

RESEARCH PRODUCT

Obesogen effects after perinatal exposure of 4,4′-sulfonyldiphenol (Bisphenol S) in C57BL/6 mice

T. Truntzer Marie-christine Chagnon Isabelle Niot Philippe Besnard Roger Rahmani Patrick Rouimi L. Ivry Del Moral Jean-françois Merlin Ludovic Le Corre Hélène Poirier

subject

Male 0301 basic medicine Leptin Bisphenol S [ SDV.TOX ] Life Sciences [q-bio]/Toxicology Adipose tissue 010501 environmental sciences Toxicology urologic and male genital diseases 01 natural sciences Polyethylene Glycols Mice chemistry.chemical_compound Pregnancy Induced Obesity Hyperinsulinemia période perinatale Obesogen Sulfones 2. Zero hunger Leptin High-Fat Diet santé humaine Lipids Energy-Balance 3. Good health Safe Alternatives obésité Adipose Tissue Prenatal Exposure Delayed Effects [SDV.TOX]Life Sciences [q-bio]/Toxicology bisphénol s Female hormones hormone substitutes and hormone antagonists medicine.medical_specialty Offspring Diet High-Fat 03 medical and health sciences Insulin resistance Phenols Internal medicine medicine Animals homéostasie lipidique Obesity RNA Messenger Triglycerides 0105 earth and related environmental sciences Dose-Response Relationship Drug Adiponectin Triglyceride Insulin-Resistance Body Weight Overweight medicine.disease bisphenol S;food contaminant;perinatal exposure;low dose;obesogen Perinatal exposure Mice Inbred C57BL Food contaminant 030104 developmental biology Endocrinology contaminant chimique Low dose Glucose Metabolism Gene Expression Regulation chemistry In-Vitro Obesogen Analogs

description

International audience; Bisphenol A were removed from consumer products and replaced by chemical substitutes such as Bisphenol S (BPS). Based on their structural similarity, BPS may be obesogen like Bisphenol A in mice. Our objective was to determine the impact of BPS on lipid homeostasis in C57B1/6 mice after perinatal and chronic exposure. Pregnant mice were exposed to BPS via the drinking water (0.2; 1.5; 50 mu g/kg bw/d). Treatment began at gestational day 0 and continued in offspring up to 23-weeks old. Then, offspring mice were fed with a standard or high fat diet. The body weight, food consumption, fat mass and energy expenditure were measured. A lipid load test was performed to check the postprandial triglyceridemia. Plasma parameters and mRNA gene expression in adipose tissues were also analysed. BPS induced overweight in male mice offspring fed with a HFD at the two highest doses. There was no change in food intake and energy expenditure. The overweight was correlated to the fat mass, hyperinsulinemia and hyperleptinemia. The plasma triglyceride clearance was significantly increased with BPS and tyloxapol (R) (triglyceride clearance inhibitor) reversed this phenomenon. BPS induced alteration in mRNA expression of marker genes involved in adipose tissue homeostasis: hormone sensitive lipase, PPAR gamma, insulin receptor, SOCS3 and adiponectin. This is the first time that BPS is described as obesogenic at low doses and after perinatal and chronic exposure in male mice. BPS potentiated the obesity induced by a HFD by inducing the lipid storage linked to faster lipid plasma clearance. (C) 2016 Elsevier Ireland Ltd. All rights reserved.

year	journal	country	edition	language
2016-05-16

10.1016/j.tox.2016.05.023 https://hal-univ-bourgogne.archives-ouvertes.fr/hal-01431231