Nicorandil induces late preconditioning against myocardial infarction in conscious rabbits

Tang, Xian Liang; Xuan, Yu Ting; Zhu, Yanqing; Shirk, Gregg; Bolli, Roberto

doi:10.1152/ajpheart.01055.2003

Cited by 22 publications

(18 citation statements)

References 74 publications

(118 reference statements)

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“…We clearly demonstrated that oral administration of nicorandil significantly increased both COX-2 mRNA and protein, resulting in the increased synthesis of prostaglandin I 2 at 6 h after treatment. These results are comparable with an earlier report that intravenous infusion of nicorandil reduced cardiac infarction in rabbits after ischemia/reperfusion injury and was accompanied by an increase in COX-2 expression 24 h after infusion [9]. Moreover, induction of GATA-4 by nicorandil preceded COX-2 induction.…”

Section: Discussionsupporting

confidence: 91%

“…Previous reports have indicated that Bcl-2 was upregulated in the myocardium of rabbits subjected to ischemia/reperfusion injury 24 h after dosing with nicorandil [9] and was upregulated by GATA-4 in doxorubicin-treated heart 24 h after doxorubicin treatment [17]. Furthermore, a recent report has indicated that nicorandil inhibited the doxorubicin-induced decrease in Bcl-2 expression [35], while our present data indicated no such effect of nicorandil at 1-6 h after treatment.…”

Section: Discussionmentioning

confidence: 99%

“…Nicorandil, a K ATP channel opener with nitrate-like activity, has been shown to have cardioprotective effects both in animals [8] and in clinical studies [9] as well as vascular endothelial protective effects [10,11]. Intravenous administration of nicorandil improved regional ventricular function after percutaneous coronary intervention in patients with ischemic heart disease [12], and it also improved the prognosis of patients with stable angina pectoris in the IONA study [13] and the JCAD study [2].…”

Section: Introductionmentioning

confidence: 99%

“…From these results, it is considered that nicorandil has a preconditioning-like cardioprotective effect against ischemic injury that acts via mitochondrial K ATP channel opening. In addition, Tang et al [9] reported that nicorandil induced cardioprotection against myocardial infarction by upregulating cardioprotective factors COX-2 and Bcl-2 in rabbits. Until now, however, the precise pharmacological profiles of cardioprotective substances induced by nicorandil have not been investigated.…”

Section: Introductionmentioning

confidence: 99%

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GATA-4 Transcription Factor Regulates Cardiac COX-2 Expression Induced by Nicorandil in Left Ventricle of Rats

Serizawa¹,

Tashiro²,

Aizawa³

et al. 2014

Pharmacology

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Background and Aims: Cardioprotective effects induced by delayed ischemic preconditioning and by nicorandil are mediated via expression of cardioprotective factors such as COX-2. The present study was undertaken to evaluate whether nicorandil could induce COX-2 in rats and to elucidate its mode of induction pharmacologically. Methods and Results: Three hours after administration of nicorandil (10 mg/kg, p.o.), COX-2 mRNA and protein were significantly increased in the left ventricle, although other cardioprotective factors (Bcl-2, eNOS, hexokinase, HSP, and iNOS) were not increased. This COX-2 induction in the left ventricle was preceded by induction of GATA-4, which was significant from 1 h after administration. Ventricular levels of 6-keto-prostaglandin F_1α were increased 6 h after administration. Although pinacidil or isosorbide dinitrate alone did not increase COX-2 mRNA, their combined application significantly increased COX-2 mRNA. Moreover, although glibenclamide or ODQ each partly inhibited the induction of COX-2 mRNA by nicorandil, their combined application significantly inhibited it. These results suggest that nicorandil induces COX-2 protein through both the activation of K_ATP channels and guanylate cyclase. Conclusion: The present study demonstrated that nicorandil induces COX-2 via GATA-4 induction in the heart through both K_ATP channel activation and its nitrate-like properties.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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GATA-4 Transcription Factor Regulates Cardiac COX-2 Expression Induced by Nicorandil in Left Ventricle of Rats

Serizawa¹,

Tashiro²,

Aizawa³

et al. 2014

Pharmacology

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“…26,54,55 Although the opening of the K-ATP channels is related to classic or first-window preconditioning, it has also been reported that nicorandil treatment upregulates the expression of cyclooxygenase-2 and Bcl-2 in MI, resulting in delayed cardioprotection similar to that afforded by the late phase of ischemic preconditioning. 56 Reports indicate that intravenous nicorandil treatment ameliorates early functional and clinical problems in patients with AMI. Ito et al 45 investigated whether intravenous nicorandil (6 mg for 24 hours after a 4-mg bolus injection) followed by oral administration of nicorandil would exert beneficial effects on microvascular function and clinical outcomes in a prospective, single-center study including 81 patients with a first anterior AMI who received successful PCI within 12 hours after symptom onset.…”

Section: Nicorandilmentioning

confidence: 99%

Pharmacological Intervention for Prevention of Left Ventricular Remodeling and Improving Prognosis in Myocardial Infarction

et al. 2008

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Early reperfusion of totally occluded coronary arteries with thrombolysis and/or percutaneous coronary intervention (PCI) for acute myocardial infarction (AMI) reduces infarct size, cardiac mortality, and in-hospital events. 1,2 Prompt reperfusion of epicardial blood flow reduces infarct size and mortality rates, in-hospital events, and reinfarction. Furthermore, successful reperfusion greatly affects the reduction in infarct size and left ventricular (LV) function. The reduction in infarct size and the improvement in LV ejection fraction may decrease mechanical stress on the noninfarcted myocardium, preventing LV remodeling, including changes in LV size and shape. 3 Preventing LV remodeling is of key importance after AMI because it may be related to a reduction in adverse cardiac events, including exacerbation of congestive heart failure and cardiac mortality rates. 4 -7 Although reperfusion therapy relieves and reduces ischemia and necrosis, the process of restoring coronary blood flow causes ischemiareperfusion injury in the ischemic myocardium, which limits the beneficial effects of reperfusion and may contribute to mortality despite successful reperfusion therapy. 8,9 Reperfusion injury is triggered by cellular and mitochondrial calcium overload, oxidant stress, endothelial dysfunction, reduction in nitric oxide production, and other factors. Because reperfusion injury limits the efficacy of reperfusion therapy alone, combined use with pharmacological intervention may moderate microcirculatory impairment and clinical outcomes. Such treatments may eventually reduce infarction size and prevent ischemic LV remodeling after AMI. Furthermore, medication in the chronic phase may affect LV remodeling and clinical prognoses. We undertook a systematic review of the literature based on pharmacological reductions in infarct size and prevention of LV remodeling, both of which may be associated with improved clinical outcomes, in cases of MI. In this review, searches through MEDLINE, LILACS, and SCIELO were the sources of information. Articles were selected by their content related to the theme.

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The Second Window of Preconditioning (SWOP) Where Are We Now?

Hausenloy

Yellon

2010

Cardiovasc Drugs Ther

138

118

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A standard ischemic preconditioning (IPC) stimulus of one or more brief episodes of non-lethal myocardial ischemia and reperfusion elicits a bi-phasic pattern of cardioprotection. The first phase manifests almost immediately following the IPC stimulus and lasts for 1-2 h, after which its effect disappears (termed classical or early IPC). The second phase of cardioprotection appears 12-24 h later and lasts for 48-72 h (termed the Second Window of Protection [SWOP] or delayed or late IPC). The cardioprotection conferred by delayed IPC is robust and ubiquitous but is not as powerful as early IPC. Although there are some similarities in the mechanisms underlying early and delayed IPC, one of the major distinctions between the two is the latter's requirement for de novo protein synthesis of distal mediators such as iNOS and COX-2 which mediate the cardioprotection 24 h after the IPC stimulus. The phenomenon of delayed IPC has been demonstrated in man using a variety of experimental models. However, its clinical application has been limited by the same factors which affect early IPC- i.e. the need to intervene before the onset of myocardial ischemia, thereby restricting its potential clinical utility to planned settings of acute myocardial ischemia-reperfusion injury such as coronary artery bypass graft surgery, cardiac transplantation and percutaneous coronary intervention. In this article, the focus will be on the origins of delayed IPC, the mechanisms underlying its delayed cardioprotective effect, and the potential areas for its clinical application.

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Nicorandil induces late preconditioning against myocardial infarction in conscious rabbits

Cited by 22 publications

References 74 publications

GATA-4 Transcription Factor Regulates Cardiac COX-2 Expression Induced by Nicorandil in Left Ventricle of Rats

GATA-4 Transcription Factor Regulates Cardiac COX-2 Expression Induced by Nicorandil in Left Ventricle of Rats

Pharmacological Intervention for Prevention of Left Ventricular Remodeling and Improving Prognosis in Myocardial Infarction

The Second Window of Preconditioning (SWOP) Where Are We Now?

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