AT2‐antagonist sensitive potentiation of angiotensin II‐induced vasoconstrictions by blockade of nitric oxide synthesis in rat renal vasculature

Muller, Catherine; Endlich, Karlhans; Barthelmebs, Mariette; Helwig, Jean-Jacques

doi:10.1038/sj.bjp.0701505

Cited by 14 publications

(34 citation statements)

References 40 publications

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“…These results differ from the full agonist activity reported on other arteries of the rat (Katusic et al 1986;Stam et al 1998;Chen et al 1999), although partial agonist activity was also observed in human uterine arteries (Jovanovic et al 1997). Apparent reduction in agonist potency and efficacy might be linked to the modulation of agonist-induced vasoconstriction by a vasodilator component via the release of endothelium-derived relaxing factors (Millette and Lamontagne 1996;Muller et al 1997) or the activation of relaxing mechanisms directly on vascular smooth muscle cells. In our hands however, oxytocin evoked no renal vasodilation after blockade of V 1A receptors and its renal vasoconstrictor response was not potentiated after blockade of oxytocin receptors.…”

Section: Discussioncontrasting

confidence: 82%

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

Loichot

Krieger

Jong

et al. 2001

Naunyn-Schmiedeberg's Archives of Pharmacology

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The aim of this study was to evaluate the renal vascular effects of oxytocin in Sprague-Dawley rats and in Brattleboro heterozygous or homozygous rats, the latter being genetically deficient in vasopressin synthesis. Studies were performed in vitro, in the isolated kidney perfused in an open circuit with a Tyrode's solution. Oxytocin induced a concentration-dependent renal vasoconstriction in Sprague-Dawley rats, at rather high concentrations (EC50=170+/-39 nM, mean +/- SEM, n=6) with a maximum response amounting to 44% of that elicited by vasopressin (increase in renal vascular resistance: 11.5+/-0.9 mmHg min ml(-1) vs. 26.2+/-2.2 mmHg min ml(-1)). Oxytocin-evoked renal vasoconstriction was abolished by SR 49059, a selective vasopressin V1A receptor antagonist (10 nM), but not by d(CH2)5[Tyr(Me)2,Thr4,Orn8,Tyr-(NH2)9] vasotocin, an oxytocin receptor antagonist (10 nM). In the presence of SR 49059, oxytocin did not induce renal vasorelaxation. Oxytocin induced renal vasoconstriction in Brattleboro homozygotes and heterozygotes (EC50=59+/-12 nM and 262+/-110 nM; Emax=7.8+/-1.1 mmHg min ml(-1) and 6.9+/-0.4 mmHg min ml(-1), n=5 respectively) with characteristics similar as observed in Sprague-Dawley rats concerning partial agonist activity, low potency and antagonism by SR 49059. Responsiveness to vasopressin did not differ in Brattleboro homozygotes and heterozygotes (EC50 approximately 0.25 nM) and was similar as we reported in Sprague-Dawley rats. These findings indicate that high concentrations of oxytocin induce renal vasoconstriction in the rat by activating vasopressin V1A receptors. The low agonist activity makes it unlikely that oxytocin can substitute functionally for vasopressin at the renal vascular V1A receptor in Brattleboro homozygous rats which are deficient in endogenous vasopressin.

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Section: Discussioncontrasting

confidence: 82%

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

Loichot

Krieger

Jong

et al. 2001

Naunyn-Schmiedeberg's Archives of Pharmacology

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“…In addition to their effect on blood pressure, long-term administration of AT1 receptor blockers results in a several-fold increase in plasma ANG II and thus a possible overstimulation of AT2 receptors [40,41,42,43]. Therefore, the effect of AT2 receptor stimulation is becoming increasingly important in both physiological and pathological situations, for example, hypertension.…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, the effect of AT2 receptor stimulation is becoming increasingly important in both physiological and pathological situations, for example, hypertension. Furthermore, a cross-talk between the two receptor subtypes (AT1 and AT2) has been described [42,43], and AT1 receptor blockade might also unmask potential effects of AT2 receptors that were overridden by AT1 receptor stimulation. This potential activation of AT2 receptors during AT1 receptor blockade may have an important role in maintaining vascular relaxation mechanisms, as previous studies have demonstrated that AT2 receptors play a vasodilator role and that selective stimulation of AT2 receptors in the presence of AT1 receptor antagonists is predicted to have a beneficial clinical effect in controlling blood pressure [44,45,46].…”

Section: Discussionmentioning

confidence: 99%

Effects of AT1 Receptor Blockade on Plasma Thromboxane A2 (TXA2) Level and Skin Microcirculation in Young Healthy Women on Low Salt Diet

Čavka

Ćosić

Grizelj

et al. 2013

Kidney Blood Press Res

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Objective: To determine the effect of AT1 receptor antagonism on skin microcirculation and plasma level of thromboxane A₂ (TXA₂). Methods: Healthy women (n=20) maintained 7 days low salt (LS) diet (intake <40 mmol Na/day) without (LS) or together with 50 mg/per day of losartan (a selective AT1 receptor inhibitor) (LS diet+losartan group). Laser Doppler flowmetry (LDF) measurements of changes in post occlusive hyperemic blood flow, plasma concentration of stable TXA₂ metabolite thromboxane B₂ (TXB₂) and plasma renin activity (PRA) aldosterone concentration, electrolytes (Na⁺, K⁺), as well as blood pressure and heart rate were determined before and after study protocols. Results: PRA and aldosterone increased significantly after 7 days of both LS diet and LS diet+losartan. LS diet or LS diet+losartan administrations had no significant effect on post-occlusion hyperemia While there was no change in TXB₂ after LS diet TXB₂ significantly increased after one week of LS+losartan compared to control levels (cTXB2 pg/mL control 101±80 vs. LS diet+losartan 190±116, p<0.05). Conclusion: These data suggest that inhibition of AT1 receptors could lead to activation of AT2 receptors, which maintain hyperemia, despite the increased level of vasoconstrictor TXA₂. These findings also suggest an important role of crosstalk between renin-angiotensin system (RAS) and arachidonic acid metabolites in the regulation of microcirculation under physiological conditions.

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“…2 Therefore, the effect of the stimulation of the AT 2 R is becoming increasingly important in both physiological and pathological situations. Furthermore, a cross-talk between the 2 receptor subtypes (AT 1 R and AT 2 R) has been described, 3,4 and AT 1 R blockade might also unmask potential effects of AT 2 Rs that were inhibited by AT 1 R stimulation.…”

mentioning

confidence: 99%

Physiological and Pathophysiological Functions of the AT ₂ Subtype Receptor of Angiotensin II

2001

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Abstract-Angiotensin II exerts a potent role in the control of hemodynamic and renal homeostasis. Angiotensin II is also a local and biologically active mediator involved in both endothelial and smooth muscle cell function acting on 2 receptor subtypes: type 1 (AT 1 R) and type 2 (AT 2 R). Whereas the key role of AT 2 R in the development of the embryo has been extensively studied, the role of AT 2 R in the adult remains more questionable, especially in humans. In vitro studies in cultured cells and in isolated segments of aorta have shown that AT 2 R stimulation could lead to the production of vasoactive substances, among which NO is certainly the most cited, suggesting that acute AT 2 R stimulation will produce vasodilation. However, in different organs or in small arteries isolated from different type of tissues, other vasoactive substances may also mediate AT 2 R-dependent dilation. Sometimes, such as in large renal arteries, AT 2 R stimulation may lead to vasoconstriction, although it is not always seen. In isolated arteries submitted to physiological conditions of pressure and flow, AT 2 R stimulation may also have a role in shear stress-induced dilation through a endothelial production of NO. Thus, when acutely stimulated, the most probable response expected from AT 2 R stimulation will be a vasodilation. Therefore, in the perspective of a chronic AT 1 R blockade in patients, overstimulation of AT 2 R might be beneficial, given their potential vasodilator effect. Concerning the possible role of AT 2 R in cardiovascular remodeling, the situation is more controversial. In vitro AT 2 R stimulation clearly inhibits cardiac and vascular smooth muscle growth and proliferation, stimulates apoptosis, and promotes extra cellular matrix synthesis. In vivo, the situation might be less beneficial if not deleterious; indeed, if chronic AT 2 R overstimulation would lead to cardiovascular hypertrophy and fibrosis, then the long-term consequences of chronic AT 1 R blockade, and thus AT 2 R overstimulation, require more in-depth analysis. (Hypertension. 2001;38: 1150-1157.)

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AT₂‐antagonist sensitive potentiation of angiotensin II‐induced vasoconstrictions by blockade of nitric oxide synthesis in rat renal vasculature

Cited by 14 publications

References 40 publications

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

Effects of AT1 Receptor Blockade on Plasma Thromboxane A<sub>2</sub> (TXA<sub>2</sub>) Level and Skin Microcirculation in Young Healthy Women on Low Salt Diet

Physiological and Pathophysiological Functions of the AT ₂ Subtype Receptor of Angiotensin II

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AT2‐antagonist sensitive potentiation of angiotensin II‐induced vasoconstrictions by blockade of nitric oxide synthesis in rat renal vasculature

Cited by 14 publications

References 40 publications

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

High concentrations of oxytocin cause vasoconstriction by activating vasopressin V 1A receptors in the isolated perfused rat kidney

Effects of AT1 Receptor Blockade on Plasma Thromboxane A<sub>2</sub> (TXA<sub>2</sub>) Level and Skin Microcirculation in Young Healthy Women on Low Salt Diet

Physiological and Pathophysiological Functions of the AT 2 Subtype Receptor of Angiotensin II

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AT₂‐antagonist sensitive potentiation of angiotensin II‐induced vasoconstrictions by blockade of nitric oxide synthesis in rat renal vasculature

Physiological and Pathophysiological Functions of the AT ₂ Subtype Receptor of Angiotensin II