Investigation of the different adrenoceptor targets of nebivolol enantiomers in rat thoracic aorta

Quang, Thuy Tran; Rozec, Bertrand; Audigane, Leslie; Gauthier, Chantal

doi:10.1111/j.1476-5381.2009.00074.x

Cited by 30 publications

(10 citation statements)

References 35 publications

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“…, Tran Quang et al . ). Thanks to its combined activity as β 1 ‐ARs antagonist and β 3 ‐ARs agonist, nebivolol is used in human clinical studies to evaluate the effects of β 3 ‐ARs activation.…”

Section: Comparative Pharmacologymentioning

confidence: 97%

β₃‐AR and the vertebrate heart: a comparative view

et al. 2015

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Recent cardiovascular research showed that, together with β1- and β2-adrenergic receptors (ARs), β3-ARs contribute to the catecholamine (CA)-dependent control of the heart. β3-ARs structure, function and ligands were investigated in mammals because of their applicative potential in human cardiovascular diseases. Only recently, the concept of a β3-AR-dependent cardiac modulation was extended to non-mammalian vertebrates, although information is still scarce and fragmentary. β3-ARs were structurally described in fish, showing a closer relationship to mammalian β1-AR than β2-AR. Functional β3-ARs are present in the cardiac tissue of teleosts and amphibians. As in mammals, activation of these receptors elicits a negative modulation of the inotropic performance through the involvement of the endothelium endocardium (EE), Gi/0 proteins and the nitric oxide (NO) signalling. This review aims to comparatively analyse data from literature on β3-ARs in mammals, with those on teleosts and amphibians. The purpose is to highlight aspects of uniformity and diversity of β3-ARs structure, ligands activity, function and signalling cascades throughout vertebrates. This may provide new perspectives aimed to clarify the biological relevance of β3-ARs in the context of the nervous and humoral control of the heart and its functional plasticity.

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Section: Comparative Pharmacologymentioning

confidence: 97%

β₃‐AR and the vertebrate heart: a comparative view

et al. 2015

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“…Stimulation of the beta 3 -AR and activation of endothelial nitric oxide synthase (eNOS) increases NO release after nebivolol treatment to cause peripheral vasodilatation and improved endothelial function (16,17). Nebivolol might also activate the beta 2 -AR (18 –20). …”

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confidence: 99%

Beta3-Adrenoreceptor Stimulation Ameliorates Myocardial Ischemia-Reperfusion Injury Via Endothelial Nitric Oxide Synthase and Neuronal Nitric Oxide Synthase Activation

Aragón

Condit

Bhushan

et al. 2011

Journal of the American College of Cardiology

116

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Objectives This paper examined whether nebivolol protects the heart via nitric oxide (NO) synthase and NO-dependent signaling in an in vivo model of acute myocardial infarction. Background Beta3-adrenergic receptor (AR) activation promotes endothelial nitric oxide synthase (eNOS) activity and NO bioavailability. We hypothesized that specific beta3-AR agonists would attenuate myocardial ischemia-reperfusion (MI/R) injury via eNOS activation and increased NO bioavailability. Methods Mice were subjected to 45 min of myocardial ischemia in vivo followed by 24 h of reperfusion (R). Nebivolol (500 ng/kg), CL 316243 (1 μg/kg), BRL-37344 (1 μg/kg), or vehicle (VEH) was administered at the time of R. Myocardial area-at-risk (AAR) and infarct size (INF)/AAR was measured at 24 h of R. Cardiac tissue and plasma were collected to evaluate eNOS phosphorylation, neuronal nitric oxide synthase (nNOS), inducible nitric oxide synthase expression, and nitrite and nitrosothiol levels. Results Nebivolol (500 ng/kg) reduced INF/AAR by 37% (p < 0.001 vs. VEH) and serum troponin-I levels from 41 ± 4 ng/ml to 25 ± 4 ng/ml (p < 0.05 vs. VEH). CL 316243 and BRL-37344 reduced INF by 39% and 42%, respectively (p < 0.001 vs. VEH). Nebivolol and CL 316243 increased eNOS phosphorylation at Ser-1177 (p < 0.05 vs. VEH) and increased nitrite and total nitrosylated protein levels. Nebivolol and CL 316243 significantly increased myocardial nNOS expression. Nebivolol failed to reduce INF after MI/R in beta3-AR−/−, eNOS−/−, and in nNOS−/− mice. Conclusions Our results indicate that beta3-AR agonists protect against MI/R injury. Furthermore, the cardioprotective effects of beta3-AR agonists are mediated by rapid eNOS and nNOS activation and increased NO bioavailability.

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“…Thus we aimed to characterize the dilator properties of nebivolol in isolated basilar arteries, in such conditions, in which the intraluminal pressure and extravascular environment were controlled. Based on previous studies [ 17 , 34 , 35 , 44 ] we have used nebivolol in a range of 10 −7 to 10 −4 M which is in accordance with a range of concentrations used by others. Our data show significant dilations of BA in response to concentration-dependent administration of nebivolol ( Fig 2 ).…”

Section: Discussionmentioning

confidence: 99%

“…For example Evangelista et al reported that antioxidant properties of nebivolol can increase the “surviving” level of NO by reducing its oxidative inactivation in human umbilical vein endothelial cells, and that beta-1/2/3 adrenoceptors may play role in the development of nebivolol-induced dilation [ 43 ]. Moreover, Georgescu et al showed nebivolol induces beta-2 adrenoceptor-mediated and Ca 2+ activated potassium channel induced hyperpolarization with the consequent relaxation in mice renal arteries [ 35 ], whereas, Tran-Quang et al has demonstrated nebivolol-induced specific, either beta-2 and beta-3 agonist or alpha-1 and beta-1 antagonist adrenoceptor-mediated relaxations in rat aortic rings [ 44 ]. It was also observed that nebivolol elicits the release of hyperpolarizing factor via activation of calcium activated potassium channels [ 34 ] that—in part—maintains vessel relaxation when eNOS (endothelial NO synthase) is inhibited [ 17 ].…”

Section: Discussionmentioning

confidence: 99%

“…Our data show significant dilations of BA in response to concentration-dependent administration of nebivolol ( Fig 2 ). Since the EC 50 is 7.8 ± 0.19 x 10 −6 M, we performed measurements with specific inhibitors near this EC 50 range in the presence of nebivolol arbitrarily at 10 −5 M. Despite the calculated pharmacologically relevant plasma concentrations in humans after taking 5 mg nebivolol orally, it is in the nM range, but it still elicits a significant decrease in systemic vascular resistance [ 44 ], and it may result in dilation in human cerebral arteries. It is also possible that smaller cerebral vessels are even more sensitivity to nebivolol, as it is a general characteristics of microvessels that their sensitivity to various drugs and stimuli increases as the size (diameter) of vessels decreases [ 51 ].…”

Section: Discussionmentioning

confidence: 99%

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The Beta-1-Receptor Blocker Nebivolol Elicits Dilation of Cerebral Arteries by Reducing Smooth Muscle [Ca2+]i

et al. 2016

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RationaleNebivolol is known to have beta-1 blocker activity, but it was also suggested that it elicits relaxation of the peripheral arteries in part via release of nitric oxide (NO). However, the effect of nebivolol on the vasomotor tone of cerebral arteries is still unclear.ObjectiveTo assess the effects of nebivolol on the diameter of isolated rat basilar arteries (BA) in control, in the presence of inhibitors of vasomotor signaling pathways of know action and hemolysed blood.Methods and ResultsVasomotor responses were measured by videomicroscopy and the intracellular Ca2+ by the Fura-2 AM ratiometric method. Under control conditions, nebivolol elicited a substantial dilation of the BA (from 216±22 to 394±20 μm; p<0.05) in a concentration-dependent manner (10−7 to 10−4 M). The dilatation was significantly reduced by endothelium denudation or by L-NAME (inhibitor of NO synthase) or by SQ22536 (adenylyl cyclase blocker). Dilatation of BA was also affected by beta-2 receptor blockade with butoxamine, but not by the guanylate cyclase blocker ODQ. Interestingly, beta-1 blockade by atenolol inhibited nebivolol-induced dilation. Also, the BKCa channel blocker iberiotoxin and KCa channel inhibitor TEA significantly reduced nebivolol-induced dilation. Nebivolol significantly reduced smooth muscle Ca2+ level, which correlated with the increases in diameters and moreover it reversed the hemolysed blood-induced constriction of BA.ConclusionsNebivolol seems to have an important dilator effect in cerebral arteries, which is mediated via several vasomotor mechanisms, converging on the reduction of smooth muscle Ca2+ levels. As such, nebivolol may be effective to improve cerebral circulation in various diseased conditions, such as hemorrhage.

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Investigation of the different adrenoceptor targets of nebivolol enantiomers in rat thoracic aorta

Cited by 30 publications

References 35 publications

β₃‐AR and the vertebrate heart: a comparative view

β₃‐AR and the vertebrate heart: a comparative view

Beta3-Adrenoreceptor Stimulation Ameliorates Myocardial Ischemia-Reperfusion Injury Via Endothelial Nitric Oxide Synthase and Neuronal Nitric Oxide Synthase Activation

The Beta-1-Receptor Blocker Nebivolol Elicits Dilation of Cerebral Arteries by Reducing Smooth Muscle [Ca2+]i

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Investigation of the different adrenoceptor targets of nebivolol enantiomers in rat thoracic aorta

Cited by 30 publications

References 35 publications

β3‐AR and the vertebrate heart: a comparative view

β3‐AR and the vertebrate heart: a comparative view

Beta3-Adrenoreceptor Stimulation Ameliorates Myocardial Ischemia-Reperfusion Injury Via Endothelial Nitric Oxide Synthase and Neuronal Nitric Oxide Synthase Activation

The Beta-1-Receptor Blocker Nebivolol Elicits Dilation of Cerebral Arteries by Reducing Smooth Muscle [Ca2+]i

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β₃‐AR and the vertebrate heart: a comparative view

β₃‐AR and the vertebrate heart: a comparative view