Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling

L. Orliaguet; T. Ejlalmanesh; A. Humbert; R. Ballaire; M. Diedisheim; J. B. Julla; D. Chokr; J. Cuenco; J. Michieletto; J. Charbit; D. Lindén; J. Boucher; C. Potier; A. Hamimi; S. Lemoine; C. Blugeon; P. Legoix; S. Lameiras; L. G. Baudrin; S. Baulande; A. Soprani; F. A. Castelli; F. Fenaille; J. P. Riveline; E. Dalmas; J. Rieusset; J. F. Gautier; N. Venteclef; F. Alzaid

doi:10.1038/s41467-022-32813-z

Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling

L. Orliaguet, T. Ejlalmanesh, A. Humbert, R. Ballaire, M. Diedisheim, J. B. Julla, D. Chokr, J. Cuenco, J. Michieletto, J. Charbit, D. Lindén, J. Boucher, C. Potier, A. Hamimi, S. Lemoine, C. Blugeon, P. Legoix, S. Lameiras, L. G. Baudrin, S. BaulandeA. Soprani, F. A. Castelli, F. Fenaille, J. P. Riveline, E. Dalmas, J. Rieusset, J. F. Gautier, N. Venteclef, F. Alzaid

Dasman Diabetes Institute

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

Adipose tissue macrophages (ATM) adapt to changes in their energetic microenvironment. Caloric excess, in a range from transient to diet-induced obesity, could result in the transition of ATMs from highly oxidative and protective to highly inflammatory and metabolically deleterious. Here, we demonstrate that Interferon Regulatory Factor 5 (IRF5) is a key regulator of macrophage oxidative capacity in response to caloric excess. ATMs from mice with genetic-deficiency of Irf5 are characterised by increased oxidative respiration and mitochondrial membrane potential. Transient inhibition of IRF5 activity leads to a similar respiratory phenotype as genomic deletion, and is reversible by reconstitution of IRF5 expression. We find that the highly oxidative nature of Irf5-deficient macrophages results from transcriptional de-repression of the mitochondrial matrix component Growth Hormone Inducible Transmembrane Protein (GHITM) gene. The Irf5-deficiency-associated high oxygen consumption could be alleviated by experimental suppression of Ghitm expression. ATMs and monocytes from patients with obesity or with type-2 diabetes retain the reciprocal regulatory relationship between Irf5 and Ghitm. Thus, our study provides insights into the mechanism of how the inflammatory transcription factor IRF5 controls physiological adaptation to diet-induced obesity via regulating mitochondrial architecture in macrophages.

Original language	English
Pages (from-to)	5089
Number of pages	1
Journal	Nature Communications
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41467-022-32813-z
State	Published - 30 Aug 2022

Funding Agency

Kuwait Foundation for the Advancement of Sciences

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1038/s41467-022-32813-z

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Orliaguet, L., Ejlalmanesh, T., Humbert, A., Ballaire, R., Diedisheim, M., Julla, J. B., Chokr, D., Cuenco, J., Michieletto, J., Charbit, J., Lindén, D., Boucher, J., Potier, C., Hamimi, A., Lemoine, S., Blugeon, C., Legoix, P., Lameiras, S., Baudrin, L. G., ... Alzaid, F. (2022). Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling. Nature Communications, 13(1), 5089. https://doi.org/10.1038/s41467-022-32813-z

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title = "Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling",

abstract = "Adipose tissue macrophages (ATM) adapt to changes in their energetic microenvironment. Caloric excess, in a range from transient to diet-induced obesity, could result in the transition of ATMs from highly oxidative and protective to highly inflammatory and metabolically deleterious. Here, we demonstrate that Interferon Regulatory Factor 5 (IRF5) is a key regulator of macrophage oxidative capacity in response to caloric excess. ATMs from mice with genetic-deficiency of Irf5 are characterised by increased oxidative respiration and mitochondrial membrane potential. Transient inhibition of IRF5 activity leads to a similar respiratory phenotype as genomic deletion, and is reversible by reconstitution of IRF5 expression. We find that the highly oxidative nature of Irf5-deficient macrophages results from transcriptional de-repression of the mitochondrial matrix component Growth Hormone Inducible Transmembrane Protein (GHITM) gene. The Irf5-deficiency-associated high oxygen consumption could be alleviated by experimental suppression of Ghitm expression. ATMs and monocytes from patients with obesity or with type-2 diabetes retain the reciprocal regulatory relationship between Irf5 and Ghitm. Thus, our study provides insights into the mechanism of how the inflammatory transcription factor IRF5 controls physiological adaptation to diet-induced obesity via regulating mitochondrial architecture in macrophages.",

author = "L. Orliaguet and T. Ejlalmanesh and A. Humbert and R. Ballaire and M. Diedisheim and Julla, \{J. B.\} and D. Chokr and J. Cuenco and J. Michieletto and J. Charbit and D. Lind{\'e}n and J. Boucher and C. Potier and A. Hamimi and S. Lemoine and C. Blugeon and P. Legoix and S. Lameiras and Baudrin, \{L. G.\} and S. Baulande and A. Soprani and Castelli, \{F. A.\} and F. Fenaille and Riveline, \{J. P.\} and E. Dalmas and J. Rieusset and Gautier, \{J. F.\} and N. Venteclef and F. Alzaid",

note = "Publisher Copyright: {\textcopyright} 2022. The Author(s).",

year = "2022",

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doi = "10.1038/s41467-022-32813-z",

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Orliaguet, L, Ejlalmanesh, T, Humbert, A, Ballaire, R, Diedisheim, M, Julla, JB, Chokr, D, Cuenco, J, Michieletto, J, Charbit, J, Lindén, D, Boucher, J, Potier, C, Hamimi, A, Lemoine, S, Blugeon, C, Legoix, P, Lameiras, S, Baudrin, LG, Baulande, S, Soprani, A, Castelli, FA, Fenaille, F, Riveline, JP, Dalmas, E, Rieusset, J, Gautier, JF, Venteclef, N & Alzaid, F 2022, 'Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling', Nature Communications, vol. 13, no. 1, pp. 5089. https://doi.org/10.1038/s41467-022-32813-z

TY - JOUR

T1 - Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling

AU - Orliaguet, L.

AU - Ejlalmanesh, T.

AU - Humbert, A.

AU - Ballaire, R.

AU - Diedisheim, M.

AU - Julla, J. B.

AU - Chokr, D.

AU - Cuenco, J.

AU - Michieletto, J.

AU - Charbit, J.

AU - Lindén, D.

AU - Boucher, J.

AU - Potier, C.

AU - Hamimi, A.

AU - Lemoine, S.

AU - Blugeon, C.

AU - Legoix, P.

AU - Lameiras, S.

AU - Baudrin, L. G.

AU - Baulande, S.

AU - Soprani, A.

AU - Castelli, F. A.

AU - Fenaille, F.

AU - Riveline, J. P.

AU - Dalmas, E.

AU - Rieusset, J.

AU - Gautier, J. F.

AU - Venteclef, N.

AU - Alzaid, F.

PY - 2022/8/30

Y1 - 2022/8/30

N2 - Adipose tissue macrophages (ATM) adapt to changes in their energetic microenvironment. Caloric excess, in a range from transient to diet-induced obesity, could result in the transition of ATMs from highly oxidative and protective to highly inflammatory and metabolically deleterious. Here, we demonstrate that Interferon Regulatory Factor 5 (IRF5) is a key regulator of macrophage oxidative capacity in response to caloric excess. ATMs from mice with genetic-deficiency of Irf5 are characterised by increased oxidative respiration and mitochondrial membrane potential. Transient inhibition of IRF5 activity leads to a similar respiratory phenotype as genomic deletion, and is reversible by reconstitution of IRF5 expression. We find that the highly oxidative nature of Irf5-deficient macrophages results from transcriptional de-repression of the mitochondrial matrix component Growth Hormone Inducible Transmembrane Protein (GHITM) gene. The Irf5-deficiency-associated high oxygen consumption could be alleviated by experimental suppression of Ghitm expression. ATMs and monocytes from patients with obesity or with type-2 diabetes retain the reciprocal regulatory relationship between Irf5 and Ghitm. Thus, our study provides insights into the mechanism of how the inflammatory transcription factor IRF5 controls physiological adaptation to diet-induced obesity via regulating mitochondrial architecture in macrophages.

AB - Adipose tissue macrophages (ATM) adapt to changes in their energetic microenvironment. Caloric excess, in a range from transient to diet-induced obesity, could result in the transition of ATMs from highly oxidative and protective to highly inflammatory and metabolically deleterious. Here, we demonstrate that Interferon Regulatory Factor 5 (IRF5) is a key regulator of macrophage oxidative capacity in response to caloric excess. ATMs from mice with genetic-deficiency of Irf5 are characterised by increased oxidative respiration and mitochondrial membrane potential. Transient inhibition of IRF5 activity leads to a similar respiratory phenotype as genomic deletion, and is reversible by reconstitution of IRF5 expression. We find that the highly oxidative nature of Irf5-deficient macrophages results from transcriptional de-repression of the mitochondrial matrix component Growth Hormone Inducible Transmembrane Protein (GHITM) gene. The Irf5-deficiency-associated high oxygen consumption could be alleviated by experimental suppression of Ghitm expression. ATMs and monocytes from patients with obesity or with type-2 diabetes retain the reciprocal regulatory relationship between Irf5 and Ghitm. Thus, our study provides insights into the mechanism of how the inflammatory transcription factor IRF5 controls physiological adaptation to diet-induced obesity via regulating mitochondrial architecture in macrophages.

UR - https://www.scopus.com/pages/publications/85136940064

U2 - 10.1038/s41467-022-32813-z

DO - 10.1038/s41467-022-32813-z

M3 - Article

C2 - 36042203

AN - SCOPUS:85136940064

VL - 13

SP - 5089

JO - Nature Communications

JF - Nature Communications

IS - 1

ER -

Early macrophage response to obesity encompasses Interferon Regulatory Factor 5 regulated mitochondrial architecture remodelling

Abstract

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UN SDGs

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