Login / Signup

Puberty as a DOHaD programming window: high-fat diet induces long-term hepatic dysfunction in male rats.

Beatriz Gonçalves Dos SantosRosiane Aparecida MirandaLucas Paulo Jacinto SaavedraFlávio Andrade FranciscoMaiara Vanusa Guedes RibeiroAnna Rebeka Oliveira FerreiraMarcos Divino Ferreira JuniorKeilah Valéria Naves CavalcanteCarlos Henrique XavierEgberto Gaspar de MouraPatrícia Cristina LisboaAriel Penha Carvalho da MotaGustavo Rodrigues PedrinoJames Andrew ArmitagePaulo Cezar de Freitas MathiasKesia Palma-RigoRodrigo Mello Gomes
Published in: Journal of developmental origins of health and disease (2023)
The aim of this study was to evaluate whether high-fat (HF) diet intake during puberty can program obesity as well as generate glucose imbalance and hepatic metabolic dysfunctions in adult life. Male Wistar rats were randomly assigned into two groups: rats fed standard chow (NF) and rats fed a HF from postnatal 30-day-old (PND30) until PND60. Then, both groups were fed a standard chow from PND60 until PND120. Euthanasia and samples collections occurred at PND120. HF animals were overweight (+11%) and had increased adiposity, hyperphagia (+12%), hyperglycaemia (+13%), hyperinsulinemia (+69%), and hypertriglyceridemia (+34%). Plasma glucose levels during intravenous glucose tolerance test (ivGTT) and intraperitoneal insulin tolerance test (ipITT) were also higher in the HF group, whereas K itt was significantly lower (-34%), suggesting reduced insulin sensitivity. In the same sense, HF animals present pancreatic islets hypertrophy and high β-cell mass. HF animals also had a significant increase in blood glucose levels during pyruvate tolerance test, indicating increased gluconeogenesis. Hepatic morphology analyses showed an increase in lipid inclusion in the HF group. Moreover, PEPCK and FAS protein expression were higher in the livers of the HF animals (+79% and + 37%, respectively). In conclusion, HF during puberty causes obese phenotype leading to glucose dyshomeostasis and nonalcoholic fatty liver disease, which can be related to the overexpression of proteins PEPCK and FAS.
Keyphrases