Reversible Blockade of Electron Transport During Ischemia Protects Mitochondria and Decreases Myocardial Injury Following Reperfusion
Overview
Affiliations
Cardiac mitochondria sustain damage during ischemia and reperfusion, contributing to cell death. The reversible blockade of electron transport during ischemia with amobarbital, an inhibitor at the rotenone site of complex I, protects mitochondria against ischemic damage. Amobarbital treatment immediately before ischemia was used to test the hypothesis that damage to mitochondrial respiration occurs mainly during ischemia and that protection of mitochondria during ischemia leads to decreased cardiac injury with reperfusion. Langendorff-perfused Fischer-344 rat hearts were treated with amobarbital (2.5 mM) or vehicle for 1 min immediately before 25 min of global ischemia. Both groups were reperfused for 30 min without additional treatment. Subsarcolemmal (SSM) and interfibrillar (IFM) populations of mitochondria were isolated after reperfusion. Ischemia and reperfusion decreased state 3 and increased state 4 respiration rate in both SSM and IFM. Amobarbital treatment protected oxidative phosphorylation measured following reperfusion and improved the coupling of respiration. Cytochrome c content measured in SSM and IFM following reperfusion decreased in untreated, but not in amobarbital-treated, hearts. H(2)O(2) release from SSM and IFM isolated from amobarbital-treated hearts during reperfusion was markedly decreased. Amobarbital treatment before ischemia improved recovery of contractile function (percentage of preischemic developed pressure: untreated 51 +/- 4%, n = 12; amobarbital 70 +/- 4%, n = 11, p < 0.01) and substantially reduced infarct size (untreated 32 +/- 2%, n = 7; amobarbital 13 +/- 2%, n = 7, p < 0.01). Thus, mitochondrial damage occurs mainly during ischemia rather than during reperfusion. Reperfusion in the setting of preserved mitochondrial respiratory function attenuates the mitochondrial release of reactive oxygen species, enhances contractile recovery, and decreases myocardial infarct size.
Zhang C, Chang X, Zhao D, He Y, Dong G, Gao L J Pharm Anal. 2025; 15(2):101051.
PMID: 39931135 PMC: 11808734. DOI: 10.1016/j.jpha.2024.101051.
Gorgey A, Khalil R, Carter W, Rivers J, Chen Q, Lesnefsky E Eur J Appl Physiol. 2024; .
PMID: 39578309 DOI: 10.1007/s00421-024-05661-6.
SPTLC3 Is Essential for Complex I Activity and Contributes to Ischemic Cardiomyopathy.
Kovilakath A, Mauro A, Valentine Y, Raucci F, Jamil M, Carter C Circulation. 2024; 150(8):622-641.
PMID: 38660786 PMC: 11333184. DOI: 10.1161/CIRCULATIONAHA.123.066879.
Chen Q, Thompson J, Hu Y, Lesnefsky E Am J Physiol Heart Circ Physiol. 2023; 326(2):H385-H395.
PMID: 38099846 PMC: 11219051. DOI: 10.1152/ajpheart.00363.2023.
Kynurenic Acid: A Novel Player in Cardioprotection against Myocardial Ischemia/Reperfusion Injuries.
Kamel R, Baetz D, Gueguen N, Lebeau L, Barbelivien A, Guihot A Pharmaceuticals (Basel). 2023; 16(10).
PMID: 37895852 PMC: 10610491. DOI: 10.3390/ph16101381.