A 5:2 Intermittent Fasting Regimen Ameliorates NASH and Fibrosis and Blunts HCC Development Via Hepatic PPARα and PCK1

Overview

Journal Cell Metab

Publisher Cell Press

Specialties Cell Biology
Endocrinology

Date 2024 May 8

PMID 38718791

Authors

Suchira Gallage

Adnan Ali

Jose Efren Barragan Avila

Nogayhan Seymen

Pierluigi Ramadori

Vera Joerke

Laimdota Zizmare

David Aicher

Indresh K Gopalsamy

Winnie Fong

Jan Kosla

Enrico Focaccia

Xin Li

Suhail Yousuf

Tjeerd Sijmonsma

Mohammad Rahbari

Katharina S Kommoss

Adrian Billeter

Sandra Prokosch

Ulrike Rothermel

Florian Mueller

Jenny Hetzer

Danijela Heide

Benjamin Schinkel

Tim Machauer

Bernd Pichler

Nisar P Malek

Thomas Longerich

Susanne Roth

Adam J Rose

Johannes Schwenck

Christoph Trautwein

Mohammad M Karimi

Mathias Heikenwalder

Affiliations

Soon will be listed here.

Abstract

The role and molecular mechanisms of intermittent fasting (IF) in non-alcoholic steatohepatitis (NASH) and its transition to hepatocellular carcinoma (HCC) are unknown. Here, we identified that an IF 5:2 regimen prevents NASH development as well as ameliorates established NASH and fibrosis without affecting total calorie intake. Furthermore, the IF 5:2 regimen blunted NASH-HCC transition when applied therapeutically. The timing, length, and number of fasting cycles as well as the type of NASH diet were critical parameters determining the benefits of fasting. Combined proteome, transcriptome, and metabolome analyses identified that peroxisome-proliferator-activated receptor alpha (PPARα) and glucocorticoid-signaling-induced PCK1 act co-operatively as hepatic executors of the fasting response. In line with this, PPARα targets and PCK1 were reduced in human NASH. Notably, only fasting initiated during the active phase of mice robustly induced glucocorticoid signaling and free-fatty-acid-induced PPARα signaling. However, hepatocyte-specific glucocorticoid receptor deletion only partially abrogated the hepatic fasting response. In contrast, the combined knockdown of Ppara and Pck1 in vivo abolished the beneficial outcomes of fasting against inflammation and fibrosis. Moreover, overexpression of Pck1 alone or together with Ppara in vivo lowered hepatic triglycerides and steatosis. Our data support the notion that the IF 5:2 regimen is a promising intervention against NASH and subsequent liver cancer.

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