Full activation of thermogenesis in brown adipocytes requires Basigin action

Author:

Rupar Kaja1,Isidor Marie S.1,Argemi‐Muntadas Lidia1,Agueda‐Oyarzabal Marina1,Plucińska Kaja1,Brown Erin L.1,Mattanovich Matthias12,Bossi Simone1,Tozzi Marco1,Tandio David1,Petersen Patricia S. S.1,Henriksen Tora I.3,Trošt Kajetan1,Hansen Jacob B.4ORCID,Gerhart‐Hines Zachary1,Nielsen Søren3,Moritz Thomas1,Emanuelli Brice1ORCID

Affiliation:

1. Novo Nordisk Foundation Center for Basic Metabolic Research, Faculty of Health and Medical Sciences University of Copenhagen Denmark

2. Novo Nordisk Foundation Center for Biosustainability Technical University of Denmark Lyngby Denmark

3. Center for Physical Activity Research, Department of Infectious Diseases, Rigshospitalet, Faculty of Health and Medical Sciences University of Copenhagen Denmark

4. Section for Cell Biology and Physiology, Department of Biology, Faculty of Science University of Copenhagen Denmark

Abstract

Exploring mechanisms responsible for brown adipose tissue's (BAT) high metabolic activity is crucial to exploit its energy‐dissipating ability for therapeutic purposes. Basigin (Bsg), a multifunctional highly glycosylated transmembrane protein, was recently proposed as one of the 98 critical markers allowing to distinguish ‘white’ and ‘brown’ adipocytes, yet its function in thermogenic brown adipocytes is unknown. Here, we report that Bsg is negatively associated with obesity in mice. By contrast, Bsg expression increased in the mature adipocyte fraction of BAT upon cold acclimation. Additionally, Bsg levels were highly induced during brown adipocyte maturation in vitro and were further increased upon β‐adrenergic stimulation in a HIF‐1α‐dependent manner. siRNA‐mediated Bsg gene silencing in cultured brown adipocytes did not impact adipogenesis nor mitochondrial function. However, a significant decrease in mitochondrial respiration, lipolysis and Ucp1 transcription was observed in adipocytes lacking Bsg, when activated by norepinephrine. Furthermore, using gas chromatography/mass spectrometry–time‐of‐flight analysis to assess the composition of cellular metabolites, we demonstrate that brown adipocytes lacking Bsg have lower levels of intracellular lactate and acetoacetate. Bsg was additionally required to regulate intracellular AcAc and tricarboxylic acid cycle intermediate levels in NE‐stimulated adipocytes. Our study highlights the critical role of Bsg in active brown adipocytes, possibly by controlling cellular metabolism.

Funder

Danish Diabetes Academy

Novo Nordisk Foundation Center for Basic Metabolic Research

TrygFonden

Publisher

Wiley

Subject

Cell Biology,Molecular Biology,Biochemistry

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