Effect of nitrovasodilators and inhibitors of nitric oxide synthase on ischaemic and reperfusion function of rat isolated hearts

Toit, Eugene F. Du; McCarthy, Joy; Miyashiro, Jody K.; Opie, Lionel H.; Brünner, Friedrich

doi:10.1038/sj.bjp.0701694

Cited by 45 publications

(27 citation statements)

References 48 publications

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“…D-NAME 100 M n ϭ 14 122.9 Ϯ 2.0 138.9 Ϯ 6.0 29.5 Ϯ 6.8 20 Ϯ 4 L-NAME 100 M n ϭ 15 127.5 Ϯ 4.9 107.9 Ϯ 9.2* 32.6 Ϯ 7.2 38 Ϯ 9 D-arginine 3 mM n ϭ 6 124.2 Ϯ 5.6 114.3 Ϯ 13.0 23.5 Ϯ 5.7 22 Ϯ 7 L-arginine 3 mM n ϭ 6 132.8 Ϯ 5.9 123.7 Ϯ 8.3 11.2 Ϯ 3.8 9 Ϯ 3 Heart rate (beats/min) D-NAME 100 M n ϭ 14 329.3 Ϯ 5.69 283.8 Ϯ 9.1 221.5 Ϯ 8.8 L-NAME 100 M n ϭ 15 326.7 Ϯ 7.4 258.7 Ϯ 10.9 196.9 Ϯ 13.9 D-arginine 3 mM n ϭ 6 323. du Toit et al, 1998), whereas concentrations above 100 M would be detrimental. Moreover, when using vasoactive concentrations of NOS inhibitors, the result is considered as beneficial in terms of postischemic recovery (Zweier et al, 1995;Wang and Zweier, 1996), or deleterious when expressed in net values (Brunner et al, 1997;du Toit et al, 1998), as was experienced in our study.…”

Section: Tablementioning

confidence: 99%

“…du Toit et al, 1998), whereas concentrations above 100 M would be detrimental. Moreover, when using vasoactive concentrations of NOS inhibitors, the result is considered as beneficial in terms of postischemic recovery (Zweier et al, 1995;Wang and Zweier, 1996), or deleterious when expressed in net values (Brunner et al, 1997;du Toit et al, 1998), as was experienced in our study. Therefore, because L-NAME treatment does not modify the duration of postischemic rhythm disturbances, we propose that the administration of 100 M L-NAME before 30 min of global ischemia and throughout reperfusion does not afford protection to the heart against postischemic injury.…”

Section: Tablementioning

confidence: 99%

“…The evolution of contractility was not different between L-or D-NAMEtreated hearts during reperfusion, but the recovery of preischemic RPP was slightly higher for the L-NAME (40 Ϯ 11%) than for the D-NAME groups (29 Ϯ 11%). Various competitive inhibitors of NOS have been shown to reduce reperfusion injury in various settings (Depré et al, 1995;Naseem et al, 1995;Zweier et al, 1995;Wang and Zweier, 1996;du Toit et al, 1998;Zhang et al, 2001). In contrast to the above-mentioned studies, some experiments reported that NOS antagonists can enhance postischemic myocardial injury (Brunner et al, 1997;du Toit et al, 1998).…”

Section: Tablementioning

confidence: 99%

“…Various competitive inhibitors of NOS have been shown to reduce reperfusion injury in various settings (Depré et al, 1995;Naseem et al, 1995;Zweier et al, 1995;Wang and Zweier, 1996;du Toit et al, 1998;Zhang et al, 2001). In contrast to the above-mentioned studies, some experiments reported that NOS antagonists can enhance postischemic myocardial injury (Brunner et al, 1997;du Toit et al, 1998). The differences may be due to the experimental models, but also to the concentration of NOS antagonists, because nonvasoactive concentrations seem to protect the heart against postischemic injury (Depré TABLE 2 Evolution of myocardial functional parameters of NAME (100 M)-or arginine (3 mM)-treated hearts for the groups receiving PBN (3 mM) as a spin trap Data are presented as means Ϯ S.E.M.…”

Section: Tablementioning

confidence: 99%

“…All three isoforms of NOS may be expressed in the heart (for review, see Shah and MacCarthy, 2000), albeit in a cell-specific manner, and the numerous physiological effects of ⅐ NO on cardiac function have been reviewed (Kelly et al, 1996). During myocardial reperfusion, the role of ⅐ NO in the development of myocardial injury has been extensively studied in different experimental models, using either NOS antagonists (Depré et al, 1995;Naseem et al, 1995;Zweier et al, 1995;Wang and Zweier, 1996;Brunner et al, 1997;du Toit et al, 1998;Zhang et al, 2001), L-arginine (Takeuchi et al, 1995;Engelman et al, 1996;Brunner et al, 1997;Wang et al, 1997;Mizuno et al, 1998), ⅐ NO donors (Brunner et al, 1997;du Toit et al, 1998), or NOS-knockout mice models (Flögel et al, 1999;Kanno et al, 2000). However, there are contradictory results concerning the possible protective or deleterious role of ⅐ NO during ischemia and reperfusion.…”

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confidence: 99%

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Postischemic Recovery and Oxidative Stress Are Independent of Nitric-Oxide Synthases Modulation in Isolated Rat Heart

Vergely¹,

Perrin-Sarrado²,

Clermont³

et al. 2002

The Journal of Pharmacology and Experimental Therapeutics

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During myocardial ischemia and reperfusion, nitric oxide ( ⅐ NO) was shown to exert either beneficial or detrimental effects. Uncoupled ⅐ NO synthases (NOS) can generate superoxide anion under suboptimal concentrations of substrate and cofactors. The aim of our study was to investigate the role of NOS modulation on 1) the evolution of functional parameters and 2) the amount of free radicals released during an ischemia-reperfusion sequence. Isolated perfused rat hearts underwent 30 min of total ischemia, followed by 30 min of reperfusion in the presence of N G -nitro-D-or L-arginine methyl ester (NAME, 100 M) or of D-or L-arginine (3 mM). Functional parameters were recorded and coronary effluents were analyzed with electron spin resonance to identify and quantify the amount of ␣-phenyl-N-tert-butylnitrone spin adducts produced during reperfusion.The antioxidant capacities of the compounds were determined with the oxygen radical absorbance capacity test. L-NAMEtreated hearts showed a reduction of coronary flow and contractile performance, although neither L-NAME nor L-arginine improved the recovery of coronary flow, left end diastolic ventricular pressure, rate pressure product, and duration of reperfusion arrhythmia, compared with their D-specific enantiomers. A large and long-lasting release of alkyl/alkoxyl radicals was detected upon reperfusion, but no differences of free radical release were observed between D-and L-NAME or D-and L-arginine treatment. These results may indicate that, in our experimental conditions, cardiac NOS might not be a major factor implicated in the oxidative burst that follows a global myocardial ischemia.

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Section: Tablementioning

confidence: 99%

Section: Tablementioning

confidence: 99%

Section: Tablementioning

confidence: 99%

Section: Tablementioning

confidence: 99%

mentioning

confidence: 99%

See 3 more Smart Citations

Postischemic Recovery and Oxidative Stress Are Independent of Nitric-Oxide Synthases Modulation in Isolated Rat Heart

Vergely¹,

Perrin-Sarrado²,

Clermont³

et al. 2002

The Journal of Pharmacology and Experimental Therapeutics

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show abstract

Cardioprotective Function of Inducible Nitric Oxide Synthase and Role of Nitric Oxide in Myocardial Ischemia and Preconditioning: an Overview of a Decade of Research

Bolli

2001

Journal of Molecular and Cellular Cardiology

555

417

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Peroxynitrite in Myocardial Ischemia-Reperfusion Injury

Lalu

Wang

Schulz

The Role of Nitric Oxide in Heart Failure

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Peroxynitrite is a highly reactive oxidant which is produced during reperfusion of the ischemic heart. The role that this molecule plays in reperfusion injury has been controversial. Many investigations have demonstrated toxic effects of peroxynitrite, whereas others have found it to be protective during reperfusion. This review surveys evidence supporting both sides and proposes that peroxynitrite is a dichotomous molecule with beneficial and detrimental effects on the reperfused heart. Its toxic effects are mediated by modification and activation of a variety of targets (including poly (ADP) ribose synthetase and matrix metalloproteinases) while its beneficial effects are primarily mediated through its reaction with thiols, resulting in the formation of NO donor compounds (S-nitrosothiols).

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Effect of nitrovasodilators and inhibitors of nitric oxide synthase on ischaemic and reperfusion function of rat isolated hearts

Cited by 45 publications

References 48 publications

Postischemic Recovery and Oxidative Stress Are Independent of Nitric-Oxide Synthases Modulation in Isolated Rat Heart

Postischemic Recovery and Oxidative Stress Are Independent of Nitric-Oxide Synthases Modulation in Isolated Rat Heart

Cardioprotective Function of Inducible Nitric Oxide Synthase and Role of Nitric Oxide in Myocardial Ischemia and Preconditioning: an Overview of a Decade of Research

Peroxynitrite in Myocardial Ischemia-Reperfusion Injury

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