Histone deacetylase 7 mediates lipopolysaccharide-inducible mitochondrial fission in macrophages

Rishika Abrol; Syeda Farhana Afroz; James Curson; Karoline Raven; Kaustav Das Gupta; Kimberley Gunther; Alun Jones; Robert Reid; Zherui Xiong; Jennifer Gunter; Jessica Engel; Christian Engwerda; Antje Blumenthal; David Fairlie; Robert Parton; Steven Zuryn; Ronan Kapetanovic; Divya Ramnath; Matthew J Sweet

doi:10.1242/jcs.264376

Article Dans Une Revue Journal of Cell Science Année : 2025

Histone deacetylase 7 mediates lipopolysaccharide-inducible mitochondrial fission in macrophages

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Rishika Abrol

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Syeda Farhana Afroz

Fonction : co premier-auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

James Curson

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Karoline Raven

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Kaustav Das Gupta

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

TLI - The Lundquist Institute for Biomedical Innovation

Kimberley Gunther

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Alun Jones

Fonction : Auteur

Institute for Molecular Bioscience

Robert Reid

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Zherui Xiong

Fonction : Auteur

Institute for Molecular Bioscience

Jennifer Gunter

Fonction : Auteur

QUT - Queensland University of Technology [Brisbane]

Jessica Engel

Fonction : Auteur

QIMR Berghofer Medical Research Institute

Christian Engwerda

Fonction : Auteur

QIMR Berghofer Medical Research Institute

Antje Blumenthal

Fonction : Auteur

David Fairlie

Fonction : Auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Australian Research Council Centre of Excellence for Innovations in Peptide and Protein Science

Robert Parton

Fonction : Auteur

Institute for Molecular Bioscience

UQ [All campuses : Brisbane, Dutton Park Gatton, Herston, St Lucia and other locations] - The University of Queensland

Steven Zuryn

Fonction : Auteur

Queensland Brain Institute

Ronan Kapetanovic

Fonction : Auteur
PersonId : 1151189
IdHAL : ronankapetanovic
ORCID : 0000-0002-2908-1014

ISP - Infectiologie et Santé Publique

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Divya Ramnath

Fonction : Auteur correspondant
PersonId : 1299413
ORCID : 0000-0002-1935-9043

Connectez-vous pour contacter l'auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Matthew J Sweet

Fonction : Auteur correspondant
PersonId : 1279970

Connectez-vous pour contacter l'auteur

Institute for Molecular Bioscience

Australian Infectious Diseases Research Centre

Résumé

Histone deacetylase 7 (HDAC7) drives several immunometabolism-related processes in macrophages including lipopolysaccharide (LPS)-inducible glycolysis and inflammatory mediator production. Using an advanced biotin ligase TurboID system in human macrophages, we report 104 candidate HDAC7 interaction partners that may contribute to its immunometabolic functions. One such protein is the mitochondrial fission-promoting GTPase dynamin-related protein 1 (DRP1), which associates with HDAC7 in cells. Using gain- and loss-of-function genetic approaches, we show that HDAC7 promotes LPS-inducible mitochondrial fission in macrophages, as well as DRP1-dependent metabolic and inflammatory responses. HDAC7 enzymatic activity was dispensable for LPS-inducible fission, as previously reported for LPS-inducible glycolysis. However, a pharmacological inhibitor of HDAC7 attenuated fission in primary human and mouse macrophages, implicating its acetyl-lysine docking function in this response. HDAC7 thus drives inducible mitochondrial fission in macrophages. Small molecules targeting the acetyl-lysine docking function of HDAC7 may have applications in preventing pathological processes driven by dysregulated mitochondrial fission.

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Soumis le : lundi 8 septembre 2025-14:49:22

Dernière modification le : mercredi 7 janvier 2026-16:24:01

Archivage à long terme le : mardi 9 décembre 2025-18:55:38

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hal-05245118 , version 1 (08-09-2025)

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CC BY 4.0 - Attribution

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HAL Id : hal-05245118 , version 1
DOI : 10.1242/jcs.264376
PUBMED : 40888031
WOS : 001602262800020

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Rishika Abrol, Syeda Farhana Afroz, James Curson, Karoline Raven, Kaustav Das Gupta, et al.. Histone deacetylase 7 mediates lipopolysaccharide-inducible mitochondrial fission in macrophages. Journal of Cell Science, 2025, 138 (19), pp.jcs264376. ⟨10.1242/jcs.264376⟩. ⟨hal-05245118⟩

Histone deacetylase 7 mediates lipopolysaccharide-inducible mitochondrial fission in macrophages

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