Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS

Edward T. Chouchani; Victoria R. Pell; Edoardo Gaude; Dunja Aksentijević; Stephanie Y. Sundier; Ellen L. Robb; Angela Logan; Sergiy M. Nadtochiy; Emily N. J. Ord; Anthony C. Smith; Filmon Eyassu; Rachel Shirley; Chou-hui Hu; Anna J. Dare; Andrew M. James; Sebastian Rogatti; Richard C. Hartley; Simon Eaton; Ana S. H. Costa; Paul S. Brookes; Sean M. Davidson; Michael R. Duchen; Kourosh Saeb-parsy; Michael J. Shattock; Alan J. Robinson; Lorraine M. Work; Christian Frezza; Thomas Krieg; Michael P. Murphy

doi:10.1038/nature13909

Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS

Edward T. Chouchani, Victoria R. Pell, Edoardo Gaude, Dunja Aksentijević, Stephanie Y. Sundier, Ellen L. Robb, Angela Logan, Sergiy M. Nadtochiy, Emily N. J. Ord, Anthony C. Smith, Filmon Eyassu, Rachel Shirley, Chou-hui Hu, Anna J. Dare, Andrew M. James, Sebastian Rogatti, Richard C. Hartley, Simon Eaton, Ana S. H. Costa, Paul S. BrookesSean M. Davidson, Michael R. Duchen, Kourosh Saeb-parsy, Michael J. Shattock, Alan J. Robinson, Lorraine M. Work, Christian Frezza, Thomas Krieg, Michael P. Murphy

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

2000 Citations (Scopus)

Abstract

Ischaemia-reperfusion injury occurs when the blood supply to an organ is disrupted and then restored, and underlies many disorders, notably heart attack and stroke. While reperfusion of ischaemic tissue is essential for survival, it also initiates oxidative damage, cell death and aberrant immune responses through the generation of mitochondrial reactive oxygen species (ROS)1,2,3,4,5. Although mitochondrial ROS production in ischaemia reperfusion is established, it has generally been considered a nonspecific response to reperfusion1,3. Here we develop a comparative in vivo metabolomic analysis, and unexpectedly identify widely conserved metabolic pathways responsible for mitochondrial ROS production during ischaemia reperfusion. We show that selective accumulation of the citric acid cycle intermediate succinate is a universal metabolic signature of ischaemia in a range of tissues and is responsible for mitochondrial ROS production during reperfusion. Ischaemic succinate accumulation arises from reversal of succinate dehydrogenase, which in turn is driven by fumarate overflow from purine nucleotide breakdown and partial reversal of the malate/aspartate shuttle. After reperfusion, the accumulated succinate is rapidly re-oxidized by succinate dehydrogenase, driving extensive ROS generation by reverse electron transport at mitochondrial complex I. Decreasing ischaemic succinate accumulation by pharmacological inhibition is sufficient to ameliorate in vivo ischaemia-reperfusion injury in murine models of heart attack and stroke. Thus, we have identified a conserved metabolic response of tissues to ischaemia and reperfusion that unifies many hitherto unconnected aspects of ischaemia-reperfusion injury. Furthermore, these findings reveal a new pathway for metabolic control of ROS production in vivo, while demonstrating that inhibition of ischaemic succinate accumulation and its oxidation after subsequent reperfusion is a potential therapeutic target to decrease ischaemia-reperfusion injury in a range of pathologies.

Original language	English
Pages (from-to)	431-435
Number of pages	4
Journal	Nature
Volume	515
Issue number	7527
Early online date	5 Nov 2014
DOIs	https://doi.org/10.1038/nature13909
Publication status	Published - 20 Nov 2014

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Chouchani, E. T., Pell, V. R., Gaude, E., Aksentijević, D., Sundier, S. Y., Robb, E. L., Logan, A., Nadtochiy, S. M., Ord, E. N. J., Smith, A. C., Eyassu, F., Shirley, R., Hu, C., Dare, A. J., James, A. M., Rogatti, S., Hartley, R. C., Eaton, S., Costa, A. S. H., ... Murphy, M. P. (2014). Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS. Nature, 515(7527), 431-435. https://doi.org/10.1038/nature13909

@article{e3ecb286ff54422ab9a913b26f3f45e3,

title = "Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS",

abstract = "Ischaemia-reperfusion injury occurs when the blood supply to an organ is disrupted and then restored, and underlies many disorders, notably heart attack and stroke. While reperfusion of ischaemic tissue is essential for survival, it also initiates oxidative damage, cell death and aberrant immune responses through the generation of mitochondrial reactive oxygen species (ROS)1,2,3,4,5. Although mitochondrial ROS production in ischaemia reperfusion is established, it has generally been considered a nonspecific response to reperfusion1,3. Here we develop a comparative in vivo metabolomic analysis, and unexpectedly identify widely conserved metabolic pathways responsible for mitochondrial ROS production during ischaemia reperfusion. We show that selective accumulation of the citric acid cycle intermediate succinate is a universal metabolic signature of ischaemia in a range of tissues and is responsible for mitochondrial ROS production during reperfusion. Ischaemic succinate accumulation arises from reversal of succinate dehydrogenase, which in turn is driven by fumarate overflow from purine nucleotide breakdown and partial reversal of the malate/aspartate shuttle. After reperfusion, the accumulated succinate is rapidly re-oxidized by succinate dehydrogenase, driving extensive ROS generation by reverse electron transport at mitochondrial complex I. Decreasing ischaemic succinate accumulation by pharmacological inhibition is sufficient to ameliorate in vivo ischaemia-reperfusion injury in murine models of heart attack and stroke. Thus, we have identified a conserved metabolic response of tissues to ischaemia and reperfusion that unifies many hitherto unconnected aspects of ischaemia-reperfusion injury. Furthermore, these findings reveal a new pathway for metabolic control of ROS production in vivo, while demonstrating that inhibition of ischaemic succinate accumulation and its oxidation after subsequent reperfusion is a potential therapeutic target to decrease ischaemia-reperfusion injury in a range of pathologies.",

author = "Chouchani, {Edward T.} and Pell, {Victoria R.} and Edoardo Gaude and Dunja Aksentijevi{\'c} and Sundier, {Stephanie Y.} and Robb, {Ellen L.} and Angela Logan and Nadtochiy, {Sergiy M.} and Ord, {Emily N. J.} and Smith, {Anthony C.} and Filmon Eyassu and Rachel Shirley and Chou-hui Hu and Dare, {Anna J.} and James, {Andrew M.} and Sebastian Rogatti and Hartley, {Richard C.} and Simon Eaton and Costa, {Ana S. H.} and Brookes, {Paul S.} and Davidson, {Sean M.} and Duchen, {Michael R.} and Kourosh Saeb-parsy and Shattock, {Michael J.} and Robinson, {Alan J.} and Work, {Lorraine M.} and Christian Frezza and Thomas Krieg and Murphy, {Michael P.}",

year = "2014",

month = nov,

day = "20",

doi = "10.1038/nature13909",

language = "English",

volume = "515",

pages = "431--435",

journal = "Nature",

issn = "0028-0836",

publisher = "Springer Nature",

number = "7527",

}

Chouchani, ET, Pell, VR, Gaude, E, Aksentijević, D, Sundier, SY, Robb, EL, Logan, A, Nadtochiy, SM, Ord, ENJ, Smith, AC, Eyassu, F, Shirley, R, Hu, C, Dare, AJ , James, AM, Rogatti, S, Hartley, RC, Eaton, S, Costa, ASH, Brookes, PS, Davidson, SM, Duchen, MR, Saeb-parsy, K, Shattock, MJ, Robinson, AJ, Work, LM, Frezza, C, Krieg, T & Murphy, MP 2014, 'Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS', Nature, vol. 515, no. 7527, pp. 431-435. https://doi.org/10.1038/nature13909

TY - JOUR

T1 - Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS

AU - Chouchani, Edward T.

AU - Pell, Victoria R.

AU - Gaude, Edoardo

AU - Aksentijević, Dunja

AU - Sundier, Stephanie Y.

AU - Robb, Ellen L.

AU - Logan, Angela

AU - Nadtochiy, Sergiy M.

AU - Ord, Emily N. J.

AU - Smith, Anthony C.

AU - Eyassu, Filmon

AU - Shirley, Rachel

AU - Hu, Chou-hui

AU - Dare, Anna J.

AU - James, Andrew M.

AU - Rogatti, Sebastian

AU - Hartley, Richard C.

AU - Eaton, Simon

AU - Costa, Ana S. H.

AU - Brookes, Paul S.

AU - Davidson, Sean M.

AU - Duchen, Michael R.

AU - Saeb-parsy, Kourosh

AU - Shattock, Michael J.

AU - Robinson, Alan J.

AU - Work, Lorraine M.

AU - Frezza, Christian

AU - Krieg, Thomas

AU - Murphy, Michael P.

PY - 2014/11/20

Y1 - 2014/11/20

N2 - Ischaemia-reperfusion injury occurs when the blood supply to an organ is disrupted and then restored, and underlies many disorders, notably heart attack and stroke. While reperfusion of ischaemic tissue is essential for survival, it also initiates oxidative damage, cell death and aberrant immune responses through the generation of mitochondrial reactive oxygen species (ROS)1,2,3,4,5. Although mitochondrial ROS production in ischaemia reperfusion is established, it has generally been considered a nonspecific response to reperfusion1,3. Here we develop a comparative in vivo metabolomic analysis, and unexpectedly identify widely conserved metabolic pathways responsible for mitochondrial ROS production during ischaemia reperfusion. We show that selective accumulation of the citric acid cycle intermediate succinate is a universal metabolic signature of ischaemia in a range of tissues and is responsible for mitochondrial ROS production during reperfusion. Ischaemic succinate accumulation arises from reversal of succinate dehydrogenase, which in turn is driven by fumarate overflow from purine nucleotide breakdown and partial reversal of the malate/aspartate shuttle. After reperfusion, the accumulated succinate is rapidly re-oxidized by succinate dehydrogenase, driving extensive ROS generation by reverse electron transport at mitochondrial complex I. Decreasing ischaemic succinate accumulation by pharmacological inhibition is sufficient to ameliorate in vivo ischaemia-reperfusion injury in murine models of heart attack and stroke. Thus, we have identified a conserved metabolic response of tissues to ischaemia and reperfusion that unifies many hitherto unconnected aspects of ischaemia-reperfusion injury. Furthermore, these findings reveal a new pathway for metabolic control of ROS production in vivo, while demonstrating that inhibition of ischaemic succinate accumulation and its oxidation after subsequent reperfusion is a potential therapeutic target to decrease ischaemia-reperfusion injury in a range of pathologies.

AB - Ischaemia-reperfusion injury occurs when the blood supply to an organ is disrupted and then restored, and underlies many disorders, notably heart attack and stroke. While reperfusion of ischaemic tissue is essential for survival, it also initiates oxidative damage, cell death and aberrant immune responses through the generation of mitochondrial reactive oxygen species (ROS)1,2,3,4,5. Although mitochondrial ROS production in ischaemia reperfusion is established, it has generally been considered a nonspecific response to reperfusion1,3. Here we develop a comparative in vivo metabolomic analysis, and unexpectedly identify widely conserved metabolic pathways responsible for mitochondrial ROS production during ischaemia reperfusion. We show that selective accumulation of the citric acid cycle intermediate succinate is a universal metabolic signature of ischaemia in a range of tissues and is responsible for mitochondrial ROS production during reperfusion. Ischaemic succinate accumulation arises from reversal of succinate dehydrogenase, which in turn is driven by fumarate overflow from purine nucleotide breakdown and partial reversal of the malate/aspartate shuttle. After reperfusion, the accumulated succinate is rapidly re-oxidized by succinate dehydrogenase, driving extensive ROS generation by reverse electron transport at mitochondrial complex I. Decreasing ischaemic succinate accumulation by pharmacological inhibition is sufficient to ameliorate in vivo ischaemia-reperfusion injury in murine models of heart attack and stroke. Thus, we have identified a conserved metabolic response of tissues to ischaemia and reperfusion that unifies many hitherto unconnected aspects of ischaemia-reperfusion injury. Furthermore, these findings reveal a new pathway for metabolic control of ROS production in vivo, while demonstrating that inhibition of ischaemic succinate accumulation and its oxidation after subsequent reperfusion is a potential therapeutic target to decrease ischaemia-reperfusion injury in a range of pathologies.

U2 - 10.1038/nature13909

DO - 10.1038/nature13909

M3 - Article

SN - 0028-0836

VL - 515

SP - 431

EP - 435

JO - Nature

JF - Nature

IS - 7527

ER -

Ischaemic accumulation of succinate controls reperfusion injury through mitochondrial ROS

Abstract

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