HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation

Donors of nitroxyl (HNO), the one electron-reduction product of nitric oxide (NO(.)), positively modulate cardiac contractility/relaxation while limiting ischemia-reperfusion (I/R) injury. The mechanisms underpinning HNO anti-ischemic effects remain poorly understood. Using isolated perfused rat hea...

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Autores principales: Mancardi, Daniele, Pagliaro, Pasquale, Ridnour, Lisa A., Tocchetti, Carlo G., Miranda, Katrina, Juhaszova, Magdalena, Sollott, Steven J., Wink, David A., Paolocci, Nazareno
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8869498/
https://www.ncbi.nlm.nih.gov/pubmed/35204265
http://dx.doi.org/10.3390/antiox11020382
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author Mancardi, Daniele
Pagliaro, Pasquale
Ridnour, Lisa A.
Tocchetti, Carlo G.
Miranda, Katrina
Juhaszova, Magdalena
Sollott, Steven J.
Wink, David A.
Paolocci, Nazareno
author_facet Mancardi, Daniele
Pagliaro, Pasquale
Ridnour, Lisa A.
Tocchetti, Carlo G.
Miranda, Katrina
Juhaszova, Magdalena
Sollott, Steven J.
Wink, David A.
Paolocci, Nazareno
author_sort Mancardi, Daniele
collection PubMed
description Donors of nitroxyl (HNO), the one electron-reduction product of nitric oxide (NO(.)), positively modulate cardiac contractility/relaxation while limiting ischemia-reperfusion (I/R) injury. The mechanisms underpinning HNO anti-ischemic effects remain poorly understood. Using isolated perfused rat hearts subjected to 30 min global ischemia/1 or 2 h reperfusion, here we tested whether, in analogy to NO(.), HNO protection requires PKCε translocation to mitochondria and K(ATP) channels activation. To this end, we compared the benefits afforded by ischemic preconditioning (IPC; 3 cycles of I/R) with those eventually granted by the NO(.) donor, diethylamine/NO, DEA/NO, and two chemically unrelated HNO donors: Angeli’s salt (AS, a prototypic donor) and isopropylamine/NO (IPA/NO, a new HNO releaser). All donors were given for 19 min before I/R injury. In control I/R hearts (1 h reperfusion), infarct size (IS) measured via tetrazolium salt staining was 66 ± 5.5% of the area at risk. Both AS and IPA/NO were as effective as IPC in reducing IS [30.7 ± 2.2 (AS), 31 ± 2.9 (IPA/NO), and 31 ± 0.8 (IPC), respectively)], whereas DEA/NO was significantly less so (36.2 ± 2.6%, p < 0.001 vs. AS, IPA/NO, or IPC). IPA/NO protection was still present after 120 min of reperfusion, and the co-infusion with the PKCε inhibitor (PKCV1-2500 nM) prevented it (IS = 30 ± 0.5 vs. 61 ± 1.8% with IPA/NO alone, p < 0.01). Irrespective of the donor, HNO anti-ischemic effects were insensitive to the K(ATP) channel inhibitor, 5-OH decanoate (5HD, 100 μM), that, in contrast, abrogated DEA/NO protection. Finally, both HNO donors markedly enhanced the mitochondrial permeability transition pore (mPTP) ROS threshold over control levels (≅35–40%), an action again insensitive to 5HD. Our study shows that HNO donors inhibit mPTP opening, thus limiting myocyte loss at reperfusion, a beneficial effect that requires PKCε translocation to the mitochondria but not mitochondrial K(+) channels activation.
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spelling pubmed-88694982022-02-25 HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation Mancardi, Daniele Pagliaro, Pasquale Ridnour, Lisa A. Tocchetti, Carlo G. Miranda, Katrina Juhaszova, Magdalena Sollott, Steven J. Wink, David A. Paolocci, Nazareno Antioxidants (Basel) Article Donors of nitroxyl (HNO), the one electron-reduction product of nitric oxide (NO(.)), positively modulate cardiac contractility/relaxation while limiting ischemia-reperfusion (I/R) injury. The mechanisms underpinning HNO anti-ischemic effects remain poorly understood. Using isolated perfused rat hearts subjected to 30 min global ischemia/1 or 2 h reperfusion, here we tested whether, in analogy to NO(.), HNO protection requires PKCε translocation to mitochondria and K(ATP) channels activation. To this end, we compared the benefits afforded by ischemic preconditioning (IPC; 3 cycles of I/R) with those eventually granted by the NO(.) donor, diethylamine/NO, DEA/NO, and two chemically unrelated HNO donors: Angeli’s salt (AS, a prototypic donor) and isopropylamine/NO (IPA/NO, a new HNO releaser). All donors were given for 19 min before I/R injury. In control I/R hearts (1 h reperfusion), infarct size (IS) measured via tetrazolium salt staining was 66 ± 5.5% of the area at risk. Both AS and IPA/NO were as effective as IPC in reducing IS [30.7 ± 2.2 (AS), 31 ± 2.9 (IPA/NO), and 31 ± 0.8 (IPC), respectively)], whereas DEA/NO was significantly less so (36.2 ± 2.6%, p < 0.001 vs. AS, IPA/NO, or IPC). IPA/NO protection was still present after 120 min of reperfusion, and the co-infusion with the PKCε inhibitor (PKCV1-2500 nM) prevented it (IS = 30 ± 0.5 vs. 61 ± 1.8% with IPA/NO alone, p < 0.01). Irrespective of the donor, HNO anti-ischemic effects were insensitive to the K(ATP) channel inhibitor, 5-OH decanoate (5HD, 100 μM), that, in contrast, abrogated DEA/NO protection. Finally, both HNO donors markedly enhanced the mitochondrial permeability transition pore (mPTP) ROS threshold over control levels (≅35–40%), an action again insensitive to 5HD. Our study shows that HNO donors inhibit mPTP opening, thus limiting myocyte loss at reperfusion, a beneficial effect that requires PKCε translocation to the mitochondria but not mitochondrial K(+) channels activation. MDPI 2022-02-14 /pmc/articles/PMC8869498/ /pubmed/35204265 http://dx.doi.org/10.3390/antiox11020382 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Mancardi, Daniele
Pagliaro, Pasquale
Ridnour, Lisa A.
Tocchetti, Carlo G.
Miranda, Katrina
Juhaszova, Magdalena
Sollott, Steven J.
Wink, David A.
Paolocci, Nazareno
HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title_full HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title_fullStr HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title_full_unstemmed HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title_short HNO Protects the Myocardium against Reperfusion Injury, Inhibiting the mPTP Opening via PKCε Activation
title_sort hno protects the myocardium against reperfusion injury, inhibiting the mptp opening via pkcε activation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8869498/
https://www.ncbi.nlm.nih.gov/pubmed/35204265
http://dx.doi.org/10.3390/antiox11020382
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