Cardiovascular drugs attenuated myocardial resistance against ischaemia-induced and reperfusion-induced injury in a rat model of repetitive occlusion

Gatzke, Nora; Güc, Nadija; Hillmeister, Philipp; Dülsner, André; Noble, Ferdinand le; Buschmann, Eva; Ingwersen, Maja; Bramlage, Peter; Buschmann, Ivo

doi:10.1136/openhrt-2018-000889

Cited by 4 publications

(4 citation statements)

References 40 publications

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“…Thus, the preservation of cell membrane integrity includes maintenance of Ca 2+ homeostasis, various types of ion exchange receptormediated mechanisms, osmotic control, and the preservation of the rich-energy phosphates. Therefore, interventions, e.g., Ca 2+ channel antagonists (Tosaki et al, 1987a;Otani et al, 2013;Becerra et al, 2016), beta-adrenergic receptor blockers (Tosaki et al, 1987b;Winchester and Pepine, 2014;Gatzke et al, 2018), and several other newly discovered molecular structures and interventions (Wilder et al, 2016;Bukhari et al, 2018;Gatzke et al, 2018), which directly or indirectly contribute to the preservation of the aforementioned processes can diminish the incidence of reperfusion-induced arrhythmias, heart failure, and sudden cardiac death. In addition, during the past three decades several new mechanisms have been proved and implicated based on molecular biological studies, as endogenous mediators, into the pathways of ischemia/reperfusion-induced injury and arrhythmogenesis, including gaseous molecules; nitric monoxide, carbon dioxide, and hydrogen sulfide.…”

Section: Ca 2+mentioning

confidence: 99%

ArrhythmoGenoPharmacoTherapy

Tósaki

2020

Front. Pharmacol.

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This review is focusing on the understanding of various factors and components governing and controlling the occurrence of ventricular arrhythmias including (i) the role of various ion channel-related changes in the action potential (AP), (ii) electrocardiograms (ECGs), (iii) some important arrhythmogenic mediators of reperfusion, and pharmacological approaches to their attenuation. The transmembrane potential in myocardial cells is depending on the cellular concentrations of several ions including sodium, calcium, and potassium on both sides of the cell membrane and active or inactive stages of ion channels. The movements of Na + , K + , and Ca 2+ via cell membranes produce various currents that provoke AP, determining the cardiac cycle and heart function. A specific channel has its own type of gate, and it is opening and closing under specific transmembrane voltage, ionic, or metabolic conditions. APs of sinoatrial (SA) node, atrioventricular (AV) node, and Purkinje cells determine the pacemaker activity (depolarization phase 4) of the heart, leading to the surface manifestation, registration, and evaluation of ECG waves in both animal models and humans. AP and ECG changes are key factors in arrhythmogenesis, and the analysis of these changes serve for the clarification of the mechanisms of antiarrhythmic drugs. The classification of antiarrhythmic drugs may be based on their electrophysiological properties emphasizing the connection between basic electrophysiological activities and antiarrhythmic properties. The review also summarizes some important mechanisms of ventricular arrhythmias in the ischemic/ reperfused myocardium and permits an assessment of antiarrhythmic potential of drugs used for pharmacotherapy under experimental and clinical conditions.

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Section: Ca 2+mentioning

confidence: 99%

ArrhythmoGenoPharmacoTherapy

Tósaki

2020

Front. Pharmacol.

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“…Furthermore, Wang and his colleagues [44] reported that the administration of NTG decreased ET-1 and CK-MB levels with the resulting prevention of myocardial pathological damage in a rat model of IR injury. Moreover, NTG could activate Na + /K + ATPase pump in the heart and thereby limits Na + and Ca 2+ overload and arrhythmias and decreases the ST segment elevation [45,46].…”

Section: Discussionmentioning

confidence: 99%

A comparative study between angiotensin receptor neprilysin inhibitor (thiorphan/irbesartan) with each of nitrate and carvedilol in a rat model of myocardial ischemic reperfusion injury

Abdulsalam

Hasanin

Mohamed

et al. 2023

Fundamemntal Clinical Pharma

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The combined angiotensin receptor neprilysin inhibitor is a promising cardioprotective pharmacological agent. This study investigated the beneficial effects of thiorphan (TH)/irbesartan (IRB), in myocardial ischemia–reperfusion (IR) injury, compared to each of nitroglycerin and carvedilol. Male Wistar rats were divided into five groups (10 rats/group): Sham, untreated I/R, TH/IRB + IR (0.1/10 mg/kg), nitroglycerin + IR (0.2 mg/kg), and carvedilol + IR (10 mg/kg). Mean arterial blood pressure, cardiac functions and arrhythmia incidence, duration and score were assessed. Cardiac levels of creatine kinase‐MB (CK‐MB), oxidative stress, endothelin‐1, ATP, Na+/K+ ATPase pump activity and mitochondria complexes activities were measured. Histopathological examination, Bcl/Bax immunohistochemistry studies and electron microscopy examination of left ventricle were performed. TH/IRB preserved the cardiac functions and mitochondrial complexes activities, mitigated cardiac damage, reduced oxidative stress and arrhythmia severity, improved the histopathological changes and decreased cardiac apoptosis. TH/IRB showed a comparable effect to each of nitroglycerin and carvedilol in alleviating the IR injury consequences. TH/IRB showed significant preservation of mitochondrial complexes activity I and II compared to nitroglycerin. TH/IRB significantly increased LVdP/dtmax and decreased oxidative stress, cardiac damage and endothelin‐1 along with increasing the ATP content, Na+/K+ ATPase pump activity and mitochondrial complexes activity when compared to carvedilol. TH/IRB showed a cardioprotective effect in reducing IR injury that is comparable to each of nitroglycerin and carvedilol that could be explained in part by its ability to preserve mitochondrial function, increase ATP, decrease oxidative stress as well as endothelin 1.

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“…Furthermore, myocardial stunning (dysfunction) may help to regulate the massive amount of ROS production in myocytes following an I/R injury ( Najafi et al 2018 ). CAT along with the SOD and GPx, play a significant role in the protection against LPO ( Gatzke et al, 2018 , Han et al, 2019 ). According to a recent study, erythrocyte reduction of CAT and SOD in acute myocardial infarction patients is caused by inactivation/alteration of these antioxidant enzymes through cross linking or exhaustion of these antioxidant enzymes through LPO ( Qu et al, 2019 , Li et al, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

“…During the reperfusion phase of I/R damage, autophagy, apoptosis, and necrosis all cause cell death ( Liu et al 2019 ). Recent years have seen significant enhancements in the protective strategies to suppress all features of post ischemic injury in cardiovascular diseases ( Gatzke et al, 2018 , Liu et al, 2019 ). Due to the scarcity of therapy options, a safer and more effective technique for developing cardiovascular drugs is urgently needed ( Badalzadeh et al, 2014 , Geldi et al, 2018 ).…”

Section: Introductionmentioning

confidence: 99%