Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission

Kensuke Tsushima; Heiko Bugger; Adam R. Wende; Jamie Soto; Gregory A. Jenson; Austin R. Tor; Rose McGlauflin; Helena C. Kenny; Yuan Zhang; Rhonda Souvenir; Xiao X. Hu; Crystal L. Sloan; Renata O. Pereira; Vitor A. Lira; Kenneth W. Spitzer; Terry L. Sharp; Kooresh I. Shoghi; Genevieve C. Sparagna; Eva A. Rog-Zielinska; Peter Kohl; Oleh Khalimonchuk; Jean E. Schaffer; E. Dale Abel

doi:10.1161/CIRCRESAHA.117.311307

Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission

Kensuke Tsushima, Heiko Bugger, Adam R. Wende, Jamie Soto, Gregory A. Jenson, Austin R. Tor, Rose McGlauflin, Helena C. Kenny, Yuan Zhang, Rhonda Souvenir, Xiao X. Hu, Crystal L. Sloan, Renata O. Pereira, Vitor A. Lira, Kenneth W. Spitzer, Terry L. Sharp, Kooresh I. Shoghi, Genevieve C. Sparagna, Eva A. Rog-Zielinska, Peter KohlOleh Khalimonchuk, Jean E. Schaffer, E. Dale Abel

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

184 Scopus citations

Abstract

Rationale: Cardiac lipotoxicity, characterized by increased uptake, oxidation, and accumulation of lipid intermediates, contributes to cardiac dysfunction in obesity and diabetes mellitus. However, mechanisms linking lipid overload and mitochondrial dysfunction are incompletely understood. Objective: To elucidate the mechanisms for mitochondrial adaptations to lipid overload in postnatal hearts in vivo. Methods and Results: Using a transgenic mouse model of cardiac lipotoxicity overexpressing ACSL1 (long-chain acyl-CoA synthetase 1) in cardiomyocytes, we show that modestly increased myocardial fatty acid uptake leads to mitochondrial structural remodeling with significant reduction in minimum diameter. This is associated with increased palmitoyl-carnitine oxidation and increased reactive oxygen species (ROS) generation in isolated mitochondria. Mitochondrial morphological changes and elevated ROS generation are also observed in palmitate-treated neonatal rat ventricular cardiomyocytes. Palmitate exposure to neonatal rat ventricular cardiomyocytes initially activates mitochondrial respiration, coupled with increased mitochondrial polarization and ATP synthesis. However, long-term exposure to palmitate (>8 hours) enhances ROS generation, which is accompanied by loss of the mitochondrial reticulum and a pattern suggesting increased mitochondrial fission. Mechanistically, lipid-induced changes in mitochondrial redox status increased mitochondrial fission by increased ubiquitination of AKAP121 (A-kinase anchor protein 121) leading to reduced phosphorylation of DRP1 (dynamin-related protein 1) at Ser637 and altered proteolytic processing of OPA1 (optic atrophy 1). Scavenging mitochondrial ROS restored mitochondrial morphology in vivo and in vitro. Conclusions: Our results reveal a molecular mechanism by which lipid overload-induced mitochondrial ROS generation causes mitochondrial dysfunction by inducing post-translational modifications of mitochondrial proteins that regulate mitochondrial dynamics. These findings provide a novel mechanism for mitochondrial dysfunction in lipotoxic cardiomyopathy.

Original language	English
Pages (from-to)	58-73
Number of pages	16
Journal	Circulation research
Volume	122
Issue number	1
DOIs	https://doi.org/10.1161/CIRCRESAHA.117.311307
State	Published - Jan 5 2018

Keywords

heart failure
metabolism
mitochondrial dynamics
oxidative stress
reactive oxygen species

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10.1161/CIRCRESAHA.117.311307

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Tsushima, K., Bugger, H., Wende, A. R., Soto, J., Jenson, G. A., Tor, A. R., McGlauflin, R., Kenny, H. C., Zhang, Y., Souvenir, R., Hu, X. X., Sloan, C. L., Pereira, R. O., Lira, V. A., Spitzer, K. W., Sharp, T. L., Shoghi, K. I., Sparagna, G. C., Rog-Zielinska, E. A., ... Abel, E. D. (2018). Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission. Circulation research, 122(1), 58-73. https://doi.org/10.1161/CIRCRESAHA.117.311307

@article{d395b203159740f3932b530a8528996e,

title = "Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission",

abstract = "Rationale: Cardiac lipotoxicity, characterized by increased uptake, oxidation, and accumulation of lipid intermediates, contributes to cardiac dysfunction in obesity and diabetes mellitus. However, mechanisms linking lipid overload and mitochondrial dysfunction are incompletely understood. Objective: To elucidate the mechanisms for mitochondrial adaptations to lipid overload in postnatal hearts in vivo. Methods and Results: Using a transgenic mouse model of cardiac lipotoxicity overexpressing ACSL1 (long-chain acyl-CoA synthetase 1) in cardiomyocytes, we show that modestly increased myocardial fatty acid uptake leads to mitochondrial structural remodeling with significant reduction in minimum diameter. This is associated with increased palmitoyl-carnitine oxidation and increased reactive oxygen species (ROS) generation in isolated mitochondria. Mitochondrial morphological changes and elevated ROS generation are also observed in palmitate-treated neonatal rat ventricular cardiomyocytes. Palmitate exposure to neonatal rat ventricular cardiomyocytes initially activates mitochondrial respiration, coupled with increased mitochondrial polarization and ATP synthesis. However, long-term exposure to palmitate (>8 hours) enhances ROS generation, which is accompanied by loss of the mitochondrial reticulum and a pattern suggesting increased mitochondrial fission. Mechanistically, lipid-induced changes in mitochondrial redox status increased mitochondrial fission by increased ubiquitination of AKAP121 (A-kinase anchor protein 121) leading to reduced phosphorylation of DRP1 (dynamin-related protein 1) at Ser637 and altered proteolytic processing of OPA1 (optic atrophy 1). Scavenging mitochondrial ROS restored mitochondrial morphology in vivo and in vitro. Conclusions: Our results reveal a molecular mechanism by which lipid overload-induced mitochondrial ROS generation causes mitochondrial dysfunction by inducing post-translational modifications of mitochondrial proteins that regulate mitochondrial dynamics. These findings provide a novel mechanism for mitochondrial dysfunction in lipotoxic cardiomyopathy.",

keywords = "heart failure, metabolism, mitochondrial dynamics, oxidative stress, reactive oxygen species",

author = "Kensuke Tsushima and Heiko Bugger and Wende, {Adam R.} and Jamie Soto and Jenson, {Gregory A.} and Tor, {Austin R.} and Rose McGlauflin and Kenny, {Helena C.} and Yuan Zhang and Rhonda Souvenir and Hu, {Xiao X.} and Sloan, {Crystal L.} and Pereira, {Renata O.} and Lira, {Vitor A.} and Spitzer, {Kenneth W.} and Sharp, {Terry L.} and Shoghi, {Kooresh I.} and Sparagna, {Genevieve C.} and Rog-Zielinska, {Eva A.} and Peter Kohl and Oleh Khalimonchuk and Schaffer, {Jean E.} and Abel, {E. Dale}",

note = "Funding Information: This work supported by Japan Heart Foundation/Bayer Yakuhin Research Grant Abroad (to K. Tsushima); American Heart Association Post-doctoral fellowship (12POST12030309; to K. Tsushima); Deutsche Forschungsgemeinschaft (DFG stipend; to H. Bugger); National Institutes of Health (R37HL042873) to K.W. Spitzer; National Institute of Health (RO1 DK064989, P20 HL113444; to J.E. Schaffer); National Institute of Health (UO1 HL087947, RO1HL108379; to E.D. Abel); Juvenile Diabetes Research Foundation (to E.D. Abel); and European Research Council Advanced Grant CardioNECT (20120314; to P. Kohl). This work utilized the Zeiss LSM710 confocal in the University of Iowa Central Microscopy Research Facilities that was purchased with funding from the NIH SIG Grant #1S10 RR025439-01, and Olympus FV100 in the University of Utah Cell Imaging Facility that was obtained using a NCRR Shared Equipment Grant # 1S10RR024761-01. Publisher Copyright: {\textcopyright} 2017 American Heart Association, Inc.",

year = "2018",

month = jan,

day = "5",

doi = "10.1161/CIRCRESAHA.117.311307",

language = "English",

volume = "122",

pages = "58--73",

journal = "Circulation research",

issn = "0009-7330",

number = "1",

}

Tsushima, K, Bugger, H, Wende, AR, Soto, J, Jenson, GA, Tor, AR, McGlauflin, R, Kenny, HC, Zhang, Y, Souvenir, R, Hu, XX, Sloan, CL, Pereira, RO, Lira, VA, Spitzer, KW, Sharp, TL, Shoghi, KI, Sparagna, GC, Rog-Zielinska, EA, Kohl, P, Khalimonchuk, O, Schaffer, JE & Abel, ED 2018, 'Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission', Circulation research, vol. 122, no. 1, pp. 58-73. https://doi.org/10.1161/CIRCRESAHA.117.311307

TY - JOUR

T1 - Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission

AU - Tsushima, Kensuke

AU - Bugger, Heiko

AU - Wende, Adam R.

AU - Soto, Jamie

AU - Jenson, Gregory A.

AU - Tor, Austin R.

AU - McGlauflin, Rose

AU - Kenny, Helena C.

AU - Zhang, Yuan

AU - Souvenir, Rhonda

AU - Hu, Xiao X.

AU - Sloan, Crystal L.

AU - Pereira, Renata O.

AU - Lira, Vitor A.

AU - Spitzer, Kenneth W.

AU - Sharp, Terry L.

AU - Shoghi, Kooresh I.

AU - Sparagna, Genevieve C.

AU - Rog-Zielinska, Eva A.

AU - Kohl, Peter

AU - Khalimonchuk, Oleh

AU - Schaffer, Jean E.

AU - Abel, E. Dale

N1 - Funding Information: This work supported by Japan Heart Foundation/Bayer Yakuhin Research Grant Abroad (to K. Tsushima); American Heart Association Post-doctoral fellowship (12POST12030309; to K. Tsushima); Deutsche Forschungsgemeinschaft (DFG stipend; to H. Bugger); National Institutes of Health (R37HL042873) to K.W. Spitzer; National Institute of Health (RO1 DK064989, P20 HL113444; to J.E. Schaffer); National Institute of Health (UO1 HL087947, RO1HL108379; to E.D. Abel); Juvenile Diabetes Research Foundation (to E.D. Abel); and European Research Council Advanced Grant CardioNECT (20120314; to P. Kohl). This work utilized the Zeiss LSM710 confocal in the University of Iowa Central Microscopy Research Facilities that was purchased with funding from the NIH SIG Grant #1S10 RR025439-01, and Olympus FV100 in the University of Utah Cell Imaging Facility that was obtained using a NCRR Shared Equipment Grant # 1S10RR024761-01. Publisher Copyright: © 2017 American Heart Association, Inc.

PY - 2018/1/5

Y1 - 2018/1/5

N2 - Rationale: Cardiac lipotoxicity, characterized by increased uptake, oxidation, and accumulation of lipid intermediates, contributes to cardiac dysfunction in obesity and diabetes mellitus. However, mechanisms linking lipid overload and mitochondrial dysfunction are incompletely understood. Objective: To elucidate the mechanisms for mitochondrial adaptations to lipid overload in postnatal hearts in vivo. Methods and Results: Using a transgenic mouse model of cardiac lipotoxicity overexpressing ACSL1 (long-chain acyl-CoA synthetase 1) in cardiomyocytes, we show that modestly increased myocardial fatty acid uptake leads to mitochondrial structural remodeling with significant reduction in minimum diameter. This is associated with increased palmitoyl-carnitine oxidation and increased reactive oxygen species (ROS) generation in isolated mitochondria. Mitochondrial morphological changes and elevated ROS generation are also observed in palmitate-treated neonatal rat ventricular cardiomyocytes. Palmitate exposure to neonatal rat ventricular cardiomyocytes initially activates mitochondrial respiration, coupled with increased mitochondrial polarization and ATP synthesis. However, long-term exposure to palmitate (>8 hours) enhances ROS generation, which is accompanied by loss of the mitochondrial reticulum and a pattern suggesting increased mitochondrial fission. Mechanistically, lipid-induced changes in mitochondrial redox status increased mitochondrial fission by increased ubiquitination of AKAP121 (A-kinase anchor protein 121) leading to reduced phosphorylation of DRP1 (dynamin-related protein 1) at Ser637 and altered proteolytic processing of OPA1 (optic atrophy 1). Scavenging mitochondrial ROS restored mitochondrial morphology in vivo and in vitro. Conclusions: Our results reveal a molecular mechanism by which lipid overload-induced mitochondrial ROS generation causes mitochondrial dysfunction by inducing post-translational modifications of mitochondrial proteins that regulate mitochondrial dynamics. These findings provide a novel mechanism for mitochondrial dysfunction in lipotoxic cardiomyopathy.

AB - Rationale: Cardiac lipotoxicity, characterized by increased uptake, oxidation, and accumulation of lipid intermediates, contributes to cardiac dysfunction in obesity and diabetes mellitus. However, mechanisms linking lipid overload and mitochondrial dysfunction are incompletely understood. Objective: To elucidate the mechanisms for mitochondrial adaptations to lipid overload in postnatal hearts in vivo. Methods and Results: Using a transgenic mouse model of cardiac lipotoxicity overexpressing ACSL1 (long-chain acyl-CoA synthetase 1) in cardiomyocytes, we show that modestly increased myocardial fatty acid uptake leads to mitochondrial structural remodeling with significant reduction in minimum diameter. This is associated with increased palmitoyl-carnitine oxidation and increased reactive oxygen species (ROS) generation in isolated mitochondria. Mitochondrial morphological changes and elevated ROS generation are also observed in palmitate-treated neonatal rat ventricular cardiomyocytes. Palmitate exposure to neonatal rat ventricular cardiomyocytes initially activates mitochondrial respiration, coupled with increased mitochondrial polarization and ATP synthesis. However, long-term exposure to palmitate (>8 hours) enhances ROS generation, which is accompanied by loss of the mitochondrial reticulum and a pattern suggesting increased mitochondrial fission. Mechanistically, lipid-induced changes in mitochondrial redox status increased mitochondrial fission by increased ubiquitination of AKAP121 (A-kinase anchor protein 121) leading to reduced phosphorylation of DRP1 (dynamin-related protein 1) at Ser637 and altered proteolytic processing of OPA1 (optic atrophy 1). Scavenging mitochondrial ROS restored mitochondrial morphology in vivo and in vitro. Conclusions: Our results reveal a molecular mechanism by which lipid overload-induced mitochondrial ROS generation causes mitochondrial dysfunction by inducing post-translational modifications of mitochondrial proteins that regulate mitochondrial dynamics. These findings provide a novel mechanism for mitochondrial dysfunction in lipotoxic cardiomyopathy.

KW - heart failure

KW - metabolism

KW - mitochondrial dynamics

KW - oxidative stress

KW - reactive oxygen species

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U2 - 10.1161/CIRCRESAHA.117.311307

DO - 10.1161/CIRCRESAHA.117.311307

M3 - Article

C2 - 29092894

AN - SCOPUS:85040187400

SN - 0009-7330

VL - 122

SP - 58

EP - 73

JO - Circulation research

JF - Circulation research

IS - 1

ER -

Mitochondrial Reactive Oxygen Species in Lipotoxic Hearts Induce Post-Translational Modifications of AKAP121, DRP1, and OPA1 That Promote Mitochondrial Fission

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