Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation

Markus Zeisbrich; Rolando E. Yanes; Hui Zhang; Ryu Watanabe; Yinyin Li; Lukas Brosig; Jison Hong; Barbara B. Wallis; John C. Giacomini; Themistocles L. Assimes; Jörg J. Goronzy; Cornelia M. Weyand

doi:10.1136/annrheumdis-2017-212647

Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation

Markus Zeisbrich, Rolando E. Yanes, Hui Zhang, Ryu Watanabe, Yinyin Li, Lukas Brosig, Jison Hong, Barbara B. Wallis, John C. Giacomini, Themistocles L. Assimes, Jörg J. Goronzy, Cornelia M. Weyand

Immunology

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33 Scopus citations

Abstract

Objectives Accelerated atherosclerotic disease typically complicates rheumatoid arthritis (rA), leading to premature cardiovascular death. Inflammatory macrophages are key effector cells in both rheumatoid synovitis and the plaques of coronary artery disease (CAd). Whether both diseases share macrophage-dependent pathogenic mechanisms is unknown. Methods patients with rA or CAd (at least one myocardial infarction) and healthy age-matched controls were recruited into the study. peripheral blood Cd14+ monocytes were differentiated into macrophages. Metabolic profiles were assessed by Seahorse Analyzer, intracellular Atp concentrations were quantified and mitochondrial protein localisation was determined by confocal image analysis. results In macrophages from patients with rA or CAd, mitochondria consumed more oxygen, generated more Atp and built tight interorganelle connections with the endoplasmic reticulum, forming mitochondria-associated membranes (MAM). Calcium transfer through MAM sites sustained mitochondrial hyperactivity and was dependent on inactivation of glycogen synthase kinase 3b (GSK3b), a serine/threonine kinase functioning as a metabolic switch. In patient-derived macrophages, inactivated pGSK3b-Ser9 co-precipitated with the mitochondrial fraction. Immunostaining of atherosclerotic plaques and synovial lesions confirmed that most macrophages had inactivated GSK3b. MAM formation and GSK3b inactivation sustained production of the collagenase cathepsin K, a macrophage effector function closely correlated with clinical disease activity in rA and CAd. conclusions re-organisation of the macrophage metabolism in patients with rA and CAd drives unopposed oxygen consumption and ultimately, excessive production of tissue-destructive enzymes. the underlying molecular defect relates to the deactivation of GSK3b, which controls mitochondrial fuel influx and as such represents a potential therapeutic target for anti-inflammatory therapy.

Original language	English (US)
Pages (from-to)	1053-1062
Number of pages	10
Journal	Annals of the rheumatic diseases
Volume	77
Issue number	7
DOIs	https://doi.org/10.1136/annrheumdis-2017-212647
State	Published - Jul 2018

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)
Rheumatology
Immunology and Allergy
Immunology

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10.1136/annrheumdis-2017-212647

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Zeisbrich, M., Yanes, R. E., Zhang, H., Watanabe, R., Li, Y., Brosig, L., Hong, J., Wallis, B. B., Giacomini, J. C., Assimes, T. L., Goronzy, J. J., & Weyand, C. M. (2018). Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation. Annals of the rheumatic diseases, 77(7), 1053-1062. https://doi.org/10.1136/annrheumdis-2017-212647

Zeisbrich, M, Yanes, RE, Zhang, H, Watanabe, R, Li, Y, Brosig, L, Hong, J, Wallis, BB, Giacomini, JC, Assimes, TL, Goronzy, JJ & Weyand, CM 2018, 'Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation', Annals of the rheumatic diseases, vol. 77, no. 7, pp. 1053-1062. https://doi.org/10.1136/annrheumdis-2017-212647

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title = "Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation",

abstract = "Objectives Accelerated atherosclerotic disease typically complicates rheumatoid arthritis (rA), leading to premature cardiovascular death. Inflammatory macrophages are key effector cells in both rheumatoid synovitis and the plaques of coronary artery disease (CAd). Whether both diseases share macrophage-dependent pathogenic mechanisms is unknown. Methods patients with rA or CAd (at least one myocardial infarction) and healthy age-matched controls were recruited into the study. peripheral blood Cd14+ monocytes were differentiated into macrophages. Metabolic profiles were assessed by Seahorse Analyzer, intracellular Atp concentrations were quantified and mitochondrial protein localisation was determined by confocal image analysis. results In macrophages from patients with rA or CAd, mitochondria consumed more oxygen, generated more Atp and built tight interorganelle connections with the endoplasmic reticulum, forming mitochondria-associated membranes (MAM). Calcium transfer through MAM sites sustained mitochondrial hyperactivity and was dependent on inactivation of glycogen synthase kinase 3b (GSK3b), a serine/threonine kinase functioning as a metabolic switch. In patient-derived macrophages, inactivated pGSK3b-Ser9 co-precipitated with the mitochondrial fraction. Immunostaining of atherosclerotic plaques and synovial lesions confirmed that most macrophages had inactivated GSK3b. MAM formation and GSK3b inactivation sustained production of the collagenase cathepsin K, a macrophage effector function closely correlated with clinical disease activity in rA and CAd. conclusions re-organisation of the macrophage metabolism in patients with rA and CAd drives unopposed oxygen consumption and ultimately, excessive production of tissue-destructive enzymes. the underlying molecular defect relates to the deactivation of GSK3b, which controls mitochondrial fuel influx and as such represents a potential therapeutic target for anti-inflammatory therapy.",

author = "Markus Zeisbrich and Yanes, {Rolando E.} and Hui Zhang and Ryu Watanabe and Yinyin Li and Lukas Brosig and Jison Hong and Wallis, {Barbara B.} and Giacomini, {John C.} and Assimes, {Themistocles L.} and Goronzy, {J{\"o}rg J.} and Weyand, {Cornelia M.}",

note = "Funding Information: Funding this work was supported by the national Institutes of Health (r01 Ar042527, r01 HL117913, r01 AI108906 and r01 AI108891, r01 AG045779, I01 Bx001669), the praespero Foundation and the Cahill discovery Fund. MZ was funded by the German research Foundation (dFG; ZE 1078/1-1). Publisher Copyright: {\textcopyright} Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved.",

year = "2018",

month = jul,

doi = "10.1136/annrheumdis-2017-212647",

language = "English (US)",

volume = "77",

pages = "1053--1062",

journal = "Annals of the rheumatic diseases",

issn = "0003-4967",

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T1 - Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation

AU - Zeisbrich, Markus

AU - Yanes, Rolando E.

AU - Zhang, Hui

AU - Watanabe, Ryu

AU - Li, Yinyin

AU - Brosig, Lukas

AU - Hong, Jison

AU - Wallis, Barbara B.

AU - Giacomini, John C.

AU - Assimes, Themistocles L.

AU - Goronzy, Jörg J.

AU - Weyand, Cornelia M.

N1 - Funding Information: Funding this work was supported by the national Institutes of Health (r01 Ar042527, r01 HL117913, r01 AI108906 and r01 AI108891, r01 AG045779, I01 Bx001669), the praespero Foundation and the Cahill discovery Fund. MZ was funded by the German research Foundation (dFG; ZE 1078/1-1). Publisher Copyright: © Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved.

PY - 2018/7

Y1 - 2018/7

N2 - Objectives Accelerated atherosclerotic disease typically complicates rheumatoid arthritis (rA), leading to premature cardiovascular death. Inflammatory macrophages are key effector cells in both rheumatoid synovitis and the plaques of coronary artery disease (CAd). Whether both diseases share macrophage-dependent pathogenic mechanisms is unknown. Methods patients with rA or CAd (at least one myocardial infarction) and healthy age-matched controls were recruited into the study. peripheral blood Cd14+ monocytes were differentiated into macrophages. Metabolic profiles were assessed by Seahorse Analyzer, intracellular Atp concentrations were quantified and mitochondrial protein localisation was determined by confocal image analysis. results In macrophages from patients with rA or CAd, mitochondria consumed more oxygen, generated more Atp and built tight interorganelle connections with the endoplasmic reticulum, forming mitochondria-associated membranes (MAM). Calcium transfer through MAM sites sustained mitochondrial hyperactivity and was dependent on inactivation of glycogen synthase kinase 3b (GSK3b), a serine/threonine kinase functioning as a metabolic switch. In patient-derived macrophages, inactivated pGSK3b-Ser9 co-precipitated with the mitochondrial fraction. Immunostaining of atherosclerotic plaques and synovial lesions confirmed that most macrophages had inactivated GSK3b. MAM formation and GSK3b inactivation sustained production of the collagenase cathepsin K, a macrophage effector function closely correlated with clinical disease activity in rA and CAd. conclusions re-organisation of the macrophage metabolism in patients with rA and CAd drives unopposed oxygen consumption and ultimately, excessive production of tissue-destructive enzymes. the underlying molecular defect relates to the deactivation of GSK3b, which controls mitochondrial fuel influx and as such represents a potential therapeutic target for anti-inflammatory therapy.

AB - Objectives Accelerated atherosclerotic disease typically complicates rheumatoid arthritis (rA), leading to premature cardiovascular death. Inflammatory macrophages are key effector cells in both rheumatoid synovitis and the plaques of coronary artery disease (CAd). Whether both diseases share macrophage-dependent pathogenic mechanisms is unknown. Methods patients with rA or CAd (at least one myocardial infarction) and healthy age-matched controls were recruited into the study. peripheral blood Cd14+ monocytes were differentiated into macrophages. Metabolic profiles were assessed by Seahorse Analyzer, intracellular Atp concentrations were quantified and mitochondrial protein localisation was determined by confocal image analysis. results In macrophages from patients with rA or CAd, mitochondria consumed more oxygen, generated more Atp and built tight interorganelle connections with the endoplasmic reticulum, forming mitochondria-associated membranes (MAM). Calcium transfer through MAM sites sustained mitochondrial hyperactivity and was dependent on inactivation of glycogen synthase kinase 3b (GSK3b), a serine/threonine kinase functioning as a metabolic switch. In patient-derived macrophages, inactivated pGSK3b-Ser9 co-precipitated with the mitochondrial fraction. Immunostaining of atherosclerotic plaques and synovial lesions confirmed that most macrophages had inactivated GSK3b. MAM formation and GSK3b inactivation sustained production of the collagenase cathepsin K, a macrophage effector function closely correlated with clinical disease activity in rA and CAd. conclusions re-organisation of the macrophage metabolism in patients with rA and CAd drives unopposed oxygen consumption and ultimately, excessive production of tissue-destructive enzymes. the underlying molecular defect relates to the deactivation of GSK3b, which controls mitochondrial fuel influx and as such represents a potential therapeutic target for anti-inflammatory therapy.

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Hypermetabolic macrophages in rheumatoid arthritis and coronary artery disease due to glycogen synthase kinase 3b inactivation

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