Reperfusion-Induced Arrhythmias Are Suppressed by Inhibition of the Angiotensin II Type 1 Receptor

Yahiro, Eiji; Ideishi, Munehito; Wang, Li Xing; Urata, Hidenori; Kumagai, Koji; Arakawa, Kikuo; Saku, Keijiro

doi:10.1159/000069722

Cited by 25 publications

(30 citation statements)

References 30 publications

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“…Angiotensin II (ANG II), formed locally by mast cell-derived renin in myocardial ischemia (Mackins et al, 2006;Reid et al, 2007), is a major NHE activator via ANG II type 1 receptors (AT 1 Rs) (Reid et al, 2004) and only a minor, indirect inhibitor via AT 2 receptors (Avkiran and Haworth, 2003). ANG II elicits reperfusion arrhythmias by a direct action (Harada et al, 1998;Yahiro et al, 2003;Iravanian and Dudley, 2008), as well as by facilitating NE release (Schömig, 1990;Meredith et al, 1991;Levi and Smith, 2000); both of these actions are AT 1 Rmediated .…”

Section: Introductionmentioning

confidence: 99%

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Hashikawa-Hobara¹,

Chan²,

Levi³

2011

J Pharmacol Exp Ther

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In severe myocardial ischemia, histamine 3 (H 3 ) receptor activation affords cardioprotection by preventing excessive norepinephrine release and arrhythmias; pivotal to this action is the inhibition of neuronal Na ϩ /H ϩ exchanger (NHE). Conversely, angiotensin II, formed locally by mast cell-derived renin, stimulates NHE via angiotensin II type 1 (AT 1 ) receptors, facilitating norepinephrine release and arrhythmias. Thus, ischemic dysfunction may depend on a balance between the NHE-modulating effects of H 3 receptors and AT 1 receptors. The purpose of this investigation was therefore to elucidate the H 3 /AT 1 receptor interaction in myocardial ischemia/reperfusion. We found that H 3 receptor blockade with clobenpropit increased norepinephrine overflow and arrhythmias in Langendorff-perfused guinea pig hearts subjected to ischemia/reperfusion. This coincided with increased neuronal AT 1 receptor expression. NHE inhibition with cariporide prevented both increases in norepinephrine release and AT 1 receptor expression. Moreover, norepinephrine release and AT 1 receptor expression were increased by the nitric oxide (NO) synthase inhibitor N G -methyl-L-arginine and the protein kinase C activator phorbol myristate acetate. H 3 receptor activation in differentiated sympathetic neuron-like PC12 cells permanently transfected with H 3 receptor cDNA caused a decrease in protein kinase C activity and AT 1 receptor protein abundance. Collectively, our findings suggest that neuronal H 3 receptor activation inhibits NHE by diminishing protein kinase C activity. Reduced NHE activity sequentially causes intracellular acidification, increased NO synthesis, and diminished AT 1 receptor expression. Thus, H 3 receptor-mediated NHE inhibition in ischemia/reperfusion not only opposes the angiotensin II-induced stimulation of NHE in cardiac sympathetic neurons, but also down-regulates AT 1 receptor expression. Cardioprotection ultimately results from the combined attenuation of angiotensin II and norepinephrine effects and alleviation of arrhythmias.

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Section: Introductionmentioning

confidence: 99%

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Hashikawa-Hobara¹,

Chan²,

Levi³

2011

J Pharmacol Exp Ther

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“…Pretreatment with the AT 1 receptor antagonists losartan or candesartan improves recovery of function and inhibits arrhythmias in Langendorff-perfused hearts exposed to global ischemia (Lee et al, 1997;Paz et al, 1998;Wang and Sjoquist, 1999). Similar protective effects of AT 1 antagonists have been reported in in vivo models subjected to transient coronary artery ligation (Harada et al, 1998;Dorge et al, 1999;Zhu et al, 2000;Yahiro et al, 2003). Other studies, however, in intact hearts have reported that AT 1 receptor antagonists actually have deleterious effects on recovery of contractile function in reperfusion (Ford et al, 1996(Ford et al, , 1998So et al, 1998).…”

mentioning

confidence: 56%

Attentuation of Cardiac Stunning by Losartan in a Cellular Model of Ischemia and Reperfusion Is Accompanied by Increased Sarcoplasmic Reticulum Ca²⁺Stores and Prevention of Cytosolic Ca²⁺Elevation

Louch

Ferrier²,

Howlett³

2004

J Pharmacol Exp Ther

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This study investigates whether protective effects of an angiotensin II type 1 receptor antagonist (losartan) in ischemia and reperfusion are mediated by actions on Ca 2ϩ cycling. Effects of exposure to losartan (10 M) in ischemia were evaluated in isolated guinea pig ventricular myocytes exposed to simulated ischemia and reperfusion at 37°C. Field-stimulated myocytes were exposed to 30 min of simulated ischemia (hypoxia, acidosis, lactate, hyperkalemia, and glucose-free) and reperfusion with Tyrode's solution for 40 min. Cell shortening was measured with a video edge detector, and Ca 2ϩ concentration was measured with fura-2. Field-stimulated myocytes exhibited stunning in reperfusion, which was abolished in cells exposed to losartan. In microelectrode studies, losartan did not alter the responses of resting potentials or action potentials to ischemia and reperfusion. In the absence of losartan, diastolic Ca 2ϩ increased in ischemia, and Ca 2ϩ transients exhibited a rebound overshoot in early reperfusion. Losartan did not affect amplitudes of Ca 2ϩ transients in ischemia but prevented elevations in diastolic Ca 2ϩ in ischemia. Furthermore, losartan prevented the overshoot of Ca 2ϩ transients in early reperfusion and increased the magnitude of Ca 2ϩ transients in late reperfusion. Sarcoplasmic reticulum (SR) Ca 2ϩ stores, determined as Ca 2ϩ released by rapid application of 10 mM caffeine, were not altered in ischemia and reperfusion. However, losartan increased SR Ca 2ϩ stores in late reperfusion, even in cells that were not exposed to simulated ischemia. We conclude that losartan abolishes stunning in reperfusion by preserving normal diastolic Ca 2ϩ in ischemia and by increasing Ca 2ϩ transients through elevation of releasable SR Ca 2ϩ

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“…The hypothesis was put forth by early experimentation, that reperfusion was a potential contributor to lethal injury of previously ischemic myocardium. 9) Protective pharmacologic agents aimed to different mechanisms administered during the reperfusion phase might be capable of limiting tissue necrosis, 10) which was demonstrated by some early experimental evidence in nonsurgical models of coronary artery occlusion-reperfusion 11,12) as well as surgical models of myocardial protection. 13) However, key aspects of inflammation and effect of antiinflammation therapy in cardiac disease are still not illustrated clearly.…”

Section: Discussionmentioning

confidence: 99%

“…[11][12][13] TNF-α synthesized greatly after myocardial I/R. Especially after myocardial reperfusion, the concentrations of TNF-α might have a more robust effusion, and the damage on the myocardium aggravated.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of TNF-^|^alpha; by Cyclophosphamide Reduces Myocardial Injury After Ischemia-Reperfusion

Jin

Chen

Wang

et al. 2013

ATCS

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Purpose: The purpose of this study was to determine whether cyclophosphamide (CP) can decrease myocardial and systemic TNF-αexpression and thus protects myocardial I/R injury. Methods: Open chest rats were subjected to 30 min of ischemia followed by 3h, 12h or 24h of reperfusion. Rats were divided into sham group, I/R group and CP group, and each group included 3 timepoint subgroups (3h, 12h and 24h). Plasma TNF-αwas measured by cytometric bead array (CBA) and immunohistochemistry was used to detect TNF-α in myocardium. Results: Compared with I/R group, rats treated with CP showed a significant difference with decreased plasma TNF-α (13.31 ± 2.62 vs 14.13 ± 5.95 pg/mL at 3 h reperfusion, 10.1 ± 2.73 vs 12.54 ± 5.00 pg/mL at 12 h reperfusion, 10.38 ± 5.59 vs 13.00 ± 3.59 pg/mL at 24 h reperfusion, p <0.05 respectively). Immunostaining was less intense with CP injection at each reperfusion time. The score of the intensity of myocardial TNF-αstaining was down regulated. Conclusions: TNF-α is expressed in the myocardium and plasma after myocardial I/R injury. CP might be a feasible strategy for anti-TNF-α to protect myocardial I/R injury.Keywords: cyclophosphamide, TNF-α, ischemia/reperfusion appeared to be associated with a reduced risk of cardiovascular disease. 1) We recently also disclosed that cyclophosphamide (CP) could improve myocardial function in rats after ischemia reperfusion injury. These findings could help to gain some insight into therapeutic potential of CP in myocardial I/R injury.2) However, the mechanism remains unclear. As we have known TNF-αis released during myocardial I/R from storage sites in tissue mast cells within the myocardium 3) and possibly also from cardiomyocyte itself 4) and the plasma inflammatory cells.5) Presently, we used open-chest ischemia-reperfusion rat model with minimal surgical trauma to further demonstrate whether down-regulation with TNF-α-related inflammatory pathways by CP could reduce myocardial injury after I/R.

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Reperfusion-Induced Arrhythmias Are Suppressed by Inhibition of the Angiotensin II Type 1 Receptor

Cited by 25 publications

References 30 publications

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Attentuation of Cardiac Stunning by Losartan in a Cellular Model of Ischemia and Reperfusion Is Accompanied by Increased Sarcoplasmic Reticulum Ca²⁺Stores and Prevention of Cytosolic Ca²⁺Elevation

Inhibition of TNF-^|^alpha; by Cyclophosphamide Reduces Myocardial Injury After Ischemia-Reperfusion

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Reperfusion-Induced Arrhythmias Are Suppressed by Inhibition of the Angiotensin II Type 1 Receptor

Cited by 25 publications

References 30 publications

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Histamine 3 Receptor Activation Reduces the Expression of Neuronal Angiotensin II Type 1 Receptors in the Heart

Attentuation of Cardiac Stunning by Losartan in a Cellular Model of Ischemia and Reperfusion Is Accompanied by Increased Sarcoplasmic Reticulum Ca2+Stores and Prevention of Cytosolic Ca2+Elevation

Inhibition of TNF-^|^alpha; by Cyclophosphamide Reduces Myocardial Injury After Ischemia-Reperfusion

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Attentuation of Cardiac Stunning by Losartan in a Cellular Model of Ischemia and Reperfusion Is Accompanied by Increased Sarcoplasmic Reticulum Ca²⁺Stores and Prevention of Cytosolic Ca²⁺Elevation