Corrupted adipose tissue endogenous myelopoiesis initiates diet-induced metabolic disease

Elodie Luche; Virginie Robert; Vincent Cuminetti; Celine Pomié; Quentin Sastourné-Arrey; Aurélie Waget; Emmanuelle Arnaud; Audrey Varin; Elodie Labit; Patrick Laharrague; Remy Burcelin; Louis Casteilla; Beatrice Cousin

doi:10.7554/eLife.23194

eLife (Jun 2017)

Corrupted adipose tissue endogenous myelopoiesis initiates diet-induced metabolic disease

Elodie Luche,
Virginie Robert,
Vincent Cuminetti,
Celine Pomié,
Quentin Sastourné-Arrey,
Aurélie Waget,
Emmanuelle Arnaud,
Audrey Varin,
Elodie Labit,
Patrick Laharrague,
Remy Burcelin,
Louis Casteilla,
Beatrice Cousin

Affiliations

Elodie Luche: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Virginie Robert: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Vincent Cuminetti: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Celine Pomié: INSERM U1048, Université de Toulouse, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Quentin Sastourné-Arrey: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Aurélie Waget: INSERM U1048, Université de Toulouse, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Emmanuelle Arnaud: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Audrey Varin: STROMALab, Université de Toulouse, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Elodie Labit: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Patrick Laharrague: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Remy Burcelin: INSERM U1048, Université de Toulouse, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Louis Casteilla: STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France
Beatrice Cousin: ORCiD; STROMALab, Université de Toulouse, CNRS ERL 5311, EFS, INP-ENVT, Inserm U1031, UPS, Toulouse, France

DOI: https://doi.org/10.7554/eLife.23194
Journal volume & issue: Vol. 6

Abstract

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Activation and increased numbers of inflammatory macrophages, in adipose tissue (AT) are deleterious in metabolic diseases. Up to now, AT macrophages (ATM) accumulation was considered to be due to blood infiltration or local proliferation, although the presence of resident hematopoietic stem/progenitor cells (Lin-/Sca+/c-Kit+; LSK phenotype) in the AT (AT-LSK) has been reported. By using transplantation of sorted AT-LSK and gain and loss of function studies we show that some of the inflammatory ATM inducing metabolic disease, originate from resident AT-LSK. Transplantation of AT-LSK sorted from high fat diet-fed (HFD) mice is sufficient to induce ATM accumulation, and to transfer metabolic disease in control mice. Conversely, the transplantation of control AT-LSK improves both AT-inflammation and glucose homeostasis in HFD mice. Our results clearly demonstrate that resident AT-LSK are one of the key point of metabolic disease, and could thus constitute a new promising therapeutic target to fight against metabolic disease.

Published in eLife

ISSN: 2050-084X (Online)
Publisher: eLife Sciences Publications Ltd
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General)
Website: https://elifesciences.org

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