Inhibition of Mevalonate Pathway Prevents Adipocyte Browning in Mice and Men by Affecting Protein Prenylation

Overview

Journal Cell Metab

Publisher Cell Press

Specialties Cell Biology
Endocrinology

Date 2018 Dec 25

PMID 30581121

Citations 40

Authors

Miroslav Balaz

Anton S Becker

Lucia Balazova

Leon Straub

Julian Muller

Gani Gashi

Claudia Irene Maushart

Wenfei Sun

Hua Dong

Caroline Moser

Carla Horvath

Vissarion Efthymiou

Yael Rachamin

Salvatore Modica

Caroline Zellweger

Sara Bacanovic

Patrik Stefanicka

Lukas Varga

Barbara Ukropcova

Milan Profant

Lennart Opitz

Ez-Zoubir Amri

Murali K Akula

Martin Bergo

Jozef Ukropec

Christian Falk

Nicola Zamboni

Matthias Johannes Betz

Irene A Burger

Christian Wolfrum

Affiliations

Soon will be listed here.

Abstract

Recent research focusing on brown adipose tissue (BAT) function emphasizes its importance in systemic metabolic homeostasis. We show here that genetic and pharmacological inhibition of the mevalonate pathway leads to reduced human and mouse brown adipocyte function in vitro and impaired adipose tissue browning in vivo. A retrospective analysis of a large patient cohort suggests an inverse correlation between statin use and active BAT in humans, while we show in a prospective clinical trial that fluvastatin reduces thermogenic gene expression in human BAT. We identify geranylgeranyl pyrophosphate as the key mevalonate pathway intermediate driving adipocyte browning in vitro and in vivo, whose effects are mediated by geranylgeranyltransferases (GGTases), enzymes catalyzing geranylgeranylation of small GTP-binding proteins, thereby regulating YAP1/TAZ signaling through F-actin modulation. Conversely, adipocyte-specific ablation of GGTase I leads to impaired adipocyte browning, reduced energy expenditure, and glucose intolerance under obesogenic conditions, highlighting the importance of this pathway in modulating brown adipocyte functionality and systemic metabolism.

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