A Macrophage-hepatocyte Glucocorticoid Receptor Axis Coordinates Fasting Ketogenesis

Overview

Journal Cell Metab

Publisher Cell Press

Specialties Cell Biology
Endocrinology

Date 2022 Feb 5

PMID 35120589

Authors

Anne Loft

Soren Fisker Schmidt

Giorgio Caratti

Ulrich Stifel

Jesper Havelund

Revathi Sekar

Yun Kwon

Alba Sulaj

Kan Kau Chow

Ana Jimena Alfaro

Thomas Schwarzmayr

Nikolaj Rittig

Mads Svart

Foivos-Filippos Tsokanos

Adriano Maida

Andreas Blutke

Annette Feuchtinger

Niels Moller

Matthias Bluher

Peter Nawroth

Julia Szendrodi

Nils J Faergeman

Anja Zeigerer

Jan Tuckermann

Stephan Herzig

Affiliations

Soon will be listed here.

Abstract

Fasting metabolism and immunity are tightly linked; however, it is largely unknown how immune cells contribute to metabolic homeostasis during fasting in healthy subjects. Here, we combined cell-type-resolved genomics and computational approaches to map crosstalk between hepatocytes and liver macrophages during fasting. We identified the glucocorticoid receptor (GR) as a key driver of fasting-induced reprogramming of the macrophage secretome including fasting-suppressed cytokines and showed that lack of macrophage GR impaired induction of ketogenesis during fasting as well as endotoxemia. Mechanistically, macrophage GR suppressed the expression of tumor necrosis factor (TNF) and promoted nuclear translocation of hepatocyte GR to activate a fat oxidation/ketogenesis-related gene program, cooperatively induced by GR and peroxisome proliferator-activated receptor alpha (PPARα) in hepatocytes. Together, our results demonstrate how resident liver macrophages directly influence ketogenesis in hepatocytes, thereby also outlining a strategy by which the immune system can set the metabolic tone during inflammatory disease and infection.

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