Therapeutic Inhibition of Acid Sensing Ion Channel 1a Recovers Heart Function After Ischemia-Reperfusion Injury
File version
Author(s)
Scheuer, Sarah E
Saez, Natalie J
Yoshikawa, Yusuke
Chiu, Han Sheng
Gao, Ling
Hicks, Mark
Villanueva, Jeanette E
Joshi, Yashutosh
Chow, Chun Yuen
Cuellar-Partida, Gabriel
Peart, Jason N
See Hoe, Louise E
Chen, Xiaoli
Sun, Yuliangzi
Griffith University Author(s)
Primary Supervisor
Other Supervisors
Editor(s)
Date
Size
File type(s)
Location
Abstract
Background: Ischemia-reperfusion injury (IRI) is one of the major risk factors implicated in morbidity and mortality associated with cardiovascular disease. During cardiac ischemia, the build-up of acidic metabolites results in decreased intracellular and extracellular pH that can reach as low as 6.0-6.5. The resulting tissue acidosis exacerbates ischemic injury and significantly impacts cardiac function. Methods: We used genetic and pharmacological methods to investigate the role of acid sensing ion channel 1a (ASIC1a) in cardiac IRI at the cellular and whole organ level. Human induced pluripotent stem cell derived cardiomyocytes (hiPSC-CMs) as well as ex vivo and in vivo models of IRI were used to test the efficacy of ASIC1a inhibitors as pre- and post-conditioning therapeutic agents. Results: Analysis of human complex trait genetics indicate that variants in the ASIC1 genetic locus are significantly associated with cardiac and cerebrovascular ischemic injuries. Using hiPSC-CMs in vitro and murine ex vivo heart models, we demonstrate that genetic ablation of ASIC1a improves cardiomyocyte viability after acute IRI. Therapeutic blockade of ASIC1a using specific and potent pharmacological inhibitors recapitulates this cardioprotective effect. We used an in vivo model of myocardial infarction (MI) and two models of ex vivo donor heart procurement and storage as clinical models to show that ASIC1a inhibition improves post-IRI cardiac viability. Use of ASIC1a inhibitors as pre- or post-conditioning agents provided equivalent cardioprotection to benchmark drugs, including the sodium-hydrogen exchange inhibitor zoniporide. At the cellular and whole organ level, we show that acute exposure to ASIC1a inhibitors has no impact on cardiac ion channels regulating baseline electromechanical coupling and physiological performance. Conclusions: Collectively, our data provide compelling evidence for a novel pharmacological strategy involving ASIC1a blockade as a cardioprotective therapy to improve the viability of hearts subjected to IRI.
Journal Title
Circulation
Conference Title
Book Title
Edition
Volume
Issue
Thesis Type
Degree Program
School
Publisher link
Patent number
Funder(s)
Grant identifier(s)
Rights Statement
Rights Statement
© 2021 American Heart Association, Inc. This is the author-manuscript version of this paper. Reproduced in accordance with the copyright policy of the publisher. Please refer to the journal's website for access to the definitive, published version.
Item Access Status
Note
Access the data
Related item(s)
Subject
Cardiovascular medicine and haematology
Clinical sciences
Health services and systems
Public health
ischemia-reperfusion injury
ion channel
cardioprotection
acidosis
Persistent link to this record
Citation
Redd, MA; Scheuer, SE; Saez, NJ; Yoshikawa, Y; Chiu, HS; Gao, L; Hicks, M; Villanueva, JE; Joshi, Y; Chow, CY; Cuellar-Partida, G; Peart, JN; See Hoe, LE; Chen, X; Sun, Y; Suen, JY; Hatch, RJ; Rollo, B; Alzubaidi, MAH; Maljevic, S; Quaife-Ryan, GA; Hudson, JE; Porrello, ER; White, MY; Cordwell, SJ; Fraser, JF; Petrou, S; Reichelt, ME; Thomas, WG; King, GF; Macdonald, PS; Palpant, NJ, Therapeutic Inhibition of Acid Sensing Ion Channel 1a Recovers Heart Function After Ischemia-Reperfusion Injury., Circulation, 2021, p. 1-40. DOI: https://doi.org/10.1161/CIRCULATIONAHA.121.054360