High-mobility group box 1 is essential for mitochondrial quality control

Daolin Tang; Rui Kang; Kristen M. Livesey; Guido Kroemer; Timothy R. Billiar; Bennett Van Houten; Herbert J. Zeh; Michael T. Lotze

doi:10.1016/j.cmet.2011.04.008

High-mobility group box 1 is essential for mitochondrial quality control

Daolin Tang, Rui Kang, Kristen M. Livesey, Guido Kroemer, Timothy R. Billiar, Bennett Van Houten, Herbert J. Zeh, Michael T. Lotze

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

242 Scopus citations

Abstract

Mitochondria are organelles centrally important for bioenergetics as well as regulation of apoptotic death in eukaryotic cells. High-mobility group box 1 (HMGB1), an evolutionarily conserved chromatin-associated protein which maintains nuclear homeostasis, is also a critical regulator of mitochondrial function and morphology. We show that heat shock protein beta-1 (HSPB1 or HSP27) is the downstream mediator of this effect. Disruption of the HSPB1 gene in embryonic fibroblasts with wild-type HMGB1 recapitulates the mitochondrial fragmentation, deficits in mitochondrial respiration, and adenosine triphosphate (ATP) synthesis observed with targeted deletion of HMGB1. Forced expression of HSPB1 reverses this phenotype in HMGB1 knockout cells. Mitochondrial effects mediated by HMGB1 regulation of HSPB1 expression serve as a defense against mitochondrial abnormality, enabling clearance and autophagy in the setting of cellular stress. Our findings reveal an essential role for HMGB1 in autophagic surveillance with important effects on mitochondrial quality control.

Original language	English (US)
Pages (from-to)	701-711
Number of pages	11
Journal	Cell Metabolism
Volume	13
Issue number	6
DOIs	https://doi.org/10.1016/j.cmet.2011.04.008
State	Published - Jun 8 2011
Externally published	Yes

ASJC Scopus subject areas

Physiology
Molecular Biology
Cell Biology

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10.1016/j.cmet.2011.04.008

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@article{5643c796b3024e76854e930cc57a8c77,

title = "High-mobility group box 1 is essential for mitochondrial quality control",

abstract = "Mitochondria are organelles centrally important for bioenergetics as well as regulation of apoptotic death in eukaryotic cells. High-mobility group box 1 (HMGB1), an evolutionarily conserved chromatin-associated protein which maintains nuclear homeostasis, is also a critical regulator of mitochondrial function and morphology. We show that heat shock protein beta-1 (HSPB1 or HSP27) is the downstream mediator of this effect. Disruption of the HSPB1 gene in embryonic fibroblasts with wild-type HMGB1 recapitulates the mitochondrial fragmentation, deficits in mitochondrial respiration, and adenosine triphosphate (ATP) synthesis observed with targeted deletion of HMGB1. Forced expression of HSPB1 reverses this phenotype in HMGB1 knockout cells. Mitochondrial effects mediated by HMGB1 regulation of HSPB1 expression serve as a defense against mitochondrial abnormality, enabling clearance and autophagy in the setting of cellular stress. Our findings reveal an essential role for HMGB1 in autophagic surveillance with important effects on mitochondrial quality control.",

author = "Daolin Tang and Rui Kang and Livesey, {Kristen M.} and Guido Kroemer and Billiar, {Timothy R.} and {Van Houten}, Bennett and Zeh, {Herbert J.} and Lotze, {Michael T.}",

note = "Funding Information: This project was funded by 1PO1CA101944 from the National Institutes of Health (M.T.L.), start-up funding from the University of Pittsburgh (D.T.) and Pennsylvania Commonwealth Universal Research Enhancement Program (B.V.H.). We thank Dr. George Hoppe (Cole Eye Institute) for pEGFPN1-HMGB1; Dr. Yoon-Jin Lee (Korea Institute of Radiological and Medical Sciences) for pcDNA4-HisMaxC-HSPB1, pcDNA4-HisMaxC-S15A, and pcDNA4-HisMaxC-S86A; Dr. Marco E. Bianchi (San Raffaele Institute, Milan, Italy) for Hmgb1 +/+ and Hmgb1 −/− MEFs; Dr. Eileen White (The Cancer Institute of New Jersey) for pEGFPC1-p62; and Drs. Patricia Loughran, Donna B. Stolz, and Simon Watkins (Center for Biologic Imaging, University of Pittsburgh Medical Center) for EM sample preparation and image analysis. Expert technical assistance from Nicole Schapiro and William Buchser, Ph.D., is appreciated. ",

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doi = "10.1016/j.cmet.2011.04.008",

language = "English (US)",

volume = "13",

pages = "701--711",

journal = "Cell Metabolism",

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T1 - High-mobility group box 1 is essential for mitochondrial quality control

AU - Tang, Daolin

AU - Kang, Rui

AU - Livesey, Kristen M.

AU - Kroemer, Guido

AU - Billiar, Timothy R.

AU - Van Houten, Bennett

AU - Zeh, Herbert J.

AU - Lotze, Michael T.

N1 - Funding Information: This project was funded by 1PO1CA101944 from the National Institutes of Health (M.T.L.), start-up funding from the University of Pittsburgh (D.T.) and Pennsylvania Commonwealth Universal Research Enhancement Program (B.V.H.). We thank Dr. George Hoppe (Cole Eye Institute) for pEGFPN1-HMGB1; Dr. Yoon-Jin Lee (Korea Institute of Radiological and Medical Sciences) for pcDNA4-HisMaxC-HSPB1, pcDNA4-HisMaxC-S15A, and pcDNA4-HisMaxC-S86A; Dr. Marco E. Bianchi (San Raffaele Institute, Milan, Italy) for Hmgb1 +/+ and Hmgb1 −/− MEFs; Dr. Eileen White (The Cancer Institute of New Jersey) for pEGFPC1-p62; and Drs. Patricia Loughran, Donna B. Stolz, and Simon Watkins (Center for Biologic Imaging, University of Pittsburgh Medical Center) for EM sample preparation and image analysis. Expert technical assistance from Nicole Schapiro and William Buchser, Ph.D., is appreciated.

PY - 2011/6/8

Y1 - 2011/6/8

N2 - Mitochondria are organelles centrally important for bioenergetics as well as regulation of apoptotic death in eukaryotic cells. High-mobility group box 1 (HMGB1), an evolutionarily conserved chromatin-associated protein which maintains nuclear homeostasis, is also a critical regulator of mitochondrial function and morphology. We show that heat shock protein beta-1 (HSPB1 or HSP27) is the downstream mediator of this effect. Disruption of the HSPB1 gene in embryonic fibroblasts with wild-type HMGB1 recapitulates the mitochondrial fragmentation, deficits in mitochondrial respiration, and adenosine triphosphate (ATP) synthesis observed with targeted deletion of HMGB1. Forced expression of HSPB1 reverses this phenotype in HMGB1 knockout cells. Mitochondrial effects mediated by HMGB1 regulation of HSPB1 expression serve as a defense against mitochondrial abnormality, enabling clearance and autophagy in the setting of cellular stress. Our findings reveal an essential role for HMGB1 in autophagic surveillance with important effects on mitochondrial quality control.

AB - Mitochondria are organelles centrally important for bioenergetics as well as regulation of apoptotic death in eukaryotic cells. High-mobility group box 1 (HMGB1), an evolutionarily conserved chromatin-associated protein which maintains nuclear homeostasis, is also a critical regulator of mitochondrial function and morphology. We show that heat shock protein beta-1 (HSPB1 or HSP27) is the downstream mediator of this effect. Disruption of the HSPB1 gene in embryonic fibroblasts with wild-type HMGB1 recapitulates the mitochondrial fragmentation, deficits in mitochondrial respiration, and adenosine triphosphate (ATP) synthesis observed with targeted deletion of HMGB1. Forced expression of HSPB1 reverses this phenotype in HMGB1 knockout cells. Mitochondrial effects mediated by HMGB1 regulation of HSPB1 expression serve as a defense against mitochondrial abnormality, enabling clearance and autophagy in the setting of cellular stress. Our findings reveal an essential role for HMGB1 in autophagic surveillance with important effects on mitochondrial quality control.

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JO - Cell Metabolism

JF - Cell Metabolism

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ER -

High-mobility group box 1 is essential for mitochondrial quality control

Abstract

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