Aldosterone induces endothelial dysfunction in resistance arteries from normotensive and hypertensive rats by increasing thromboxane A<sub>2</sub> and prostacyclin

Xavier, Fabiano E.; Aras-López, Rosa; Arroyo-Villa, Irene; Campo, Lara del; Salaíces, Mercedes; Rossoni, Luciana Venturini; Ferrer, Mercedes; Balfagón, Gloria

doi:10.1038/bjp.2008.200

Cited by 71 publications

(102 citation statements)

References 26 publications

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“…6 Aldosteroneinduced kidney injury is likely to be multifactorial, including its effect on systemic blood pressure, renal vasculature, local inflammation, and fibrosis. Various potential pathways and mediators have been proposed, including plasminogen activator inhibitor-1, 13 transforming growth factor-β1, 14 reactive oxygen species, 15 angiotensin type 1 receptor, 16 vascular endothelial growth factor, 17 as well as changes in vascular smooth muscle 18 and endothelial cells 19 (Table 1). In addition to the traditional nuclear receptor and transcription mediation pathway, aldosterone could alter a number of cellular signaling within minutes by the presumably "non-genomic" actions.…”

Section: Aldosterone As a Mediator Of Kidney Injurymentioning

confidence: 99%

Mineralocorticoid Receptor Antagonist for Renal Protection

King-Wing

Szeto

2012

Renal Failure

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The renin-angiotensin system (RAS) plays an important role in the pathophysiology of cardiovascular and renal diseases. In chronic kidney disease (CKD), blockade of RAS by angiotensin-converting enzyme inhibitor (ACEI) or angiotensin receptor blocker (ARB) has been shown to reduce proteinuria and retard the progression of renal function deterioration. However, aldosterone, another key hormone of the RAS, is not directly targeted by ACEI or ARB. Hyperaldosteronism, apart from promoting sodium and fluid retention, causes inflammation and fibrosis in the heart and kidney. Studies have shown that although plasma aldosterone level shows an initial decrease following ACEI or ARB treatment, it returns to pretreatment level or even increases paradoxically after prolonged treatment. This "aldosterone breakthrough" forms the basis of adding mineralocorticoid receptor (MR) antagonist on top of ACEI or ARB for renal protection. New insights into the pathophysiological role of aldosterone in CKD further expands its potential indications, and there was a growing body of evidence in the past 10 years, which showed a substantial antiproteinuric effect and possibly a considerable renoprotective effect of MR antagonist. Since aldosterone does not act on the efferent glomerular arteriole and has no effect on intraglomerular hemodynamics, the very fact that MR antagonist ameliorates proteinuria sheds light on the physiology of glomerular permeability barrier. This review summarizes the data regarding the theoretical benefit as well as clinical use of MR antagonist in renal diseases.

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Section: Aldosterone As a Mediator Of Kidney Injurymentioning

confidence: 99%

Mineralocorticoid Receptor Antagonist for Renal Protection

King-Wing

Szeto

2012

Renal Failure

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“…In addition, while mice are commonly used as models to study human diseases, such as hypertension, the exact role of PGI 2 synthesis in their renal arteries still remains to be clearly elucidated. Moreover, there is considerable inconsistency regarding the role of each of the two COX isoforms in regulating vasomotor reactions, including those of renal vasculature (6,8,12,17,27,29,34,35,37,38,40), possibly in part due to the use of isoform-selective COX inhibitors that might have effects independent of their intended targets (2,3,20,26).Therefore, the aim of this study was to determine whether PGI 2 evokes contraction in mouse renal arteries and, if so, how TP and/or IP receptors function in the vessel. In addition, experiments were performed to determine how the genetic deficiency of COX-1 (COX-1 Ϫ/Ϫ ) influences on the in vitro PGI 2 synthesis and/or vasomotor reaction.…”

mentioning

confidence: 99%

“…On the other hand, studies also indicate that the endothelial COX-mediated metabolism generates vasoconstrictor products that act on thromboxane-prostanoid (TP) receptors to mediate vasoconstriction (9,14,16,28,30,32,43). Interestingly, PGI 2 can also activate smooth muscle TP receptors (11,21,22,36,38). This has been explained by an excessive production of PGI 2 and/or dysfunction of IP receptors found in conditions such as hypertension (11,36,38).…”

mentioning

confidence: 99%

“…Interestingly, PGI 2 can also activate smooth muscle TP receptors (11,21,22,36,38). This has been explained by an excessive production of PGI 2 and/or dysfunction of IP receptors found in conditions such as hypertension (11,36,38). Moreover, both TP and IP receptors may concomitantly modulate the vasomotor reaction to PGI 2 ; hence, in vessels with limited functional IP receptors the process of PGI 2 synthesis itself is suggested to mediate a vasoconstrictor response even under normal physiological conditions (7,19,21,30).…”

mentioning

confidence: 99%

“…Moreover, our recent studies suggest that in porcine interlobular renal arteries COX-1-mediated endothelial PGI 2 synthesis is responsible for endothelium-dependent vasoconstrictor activity evoked by agonists, such as bradykinin (22). On the other hand, the effect of PGI 2 on a given vascular bed may vary considerably between species (19,38). In addition, while mice are commonly used as models to study human diseases, such as hypertension, the exact role of PGI 2 synthesis in their renal arteries still remains to be clearly elucidated.…”

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confidence: 99%

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A vasoconstrictor role for cyclooxygenase-1-mediated prostacyclin synthesis in mouse renal arteries

Liu

Zhang

Zhu

et al. 2013

American Journal of Physiology-Renal Physiology

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This study was to determine whether prostacyclin [prostaglandin I 2 (PGI2)] evokes mouse renal vasoconstriction and, if so, the underlying mechanism(s) and how its synthesis via cyclooxygenase-1 (COX-1) influences local vasomotor reaction. Experiments were performed on vessels from C57BL/6 mice and/or those with COX-1 deficiency (COX-1 Ϫ/Ϫ ). Results showed that in renal arteries PGI2 evoked contraction more potently than in carotid arteries, where COX-1 is suggested to mediate prominent endothelium-dependent contraction. A similar result was observed with the thromboxane-prostanoid (TP) receptor agonist U46619. However, in renal arteries TP receptor antagonism, which inhibited the contraction, did not result in any relaxation in response to PGI2. Moreover, we noted that the endothelial muscarinic receptor agonist ACh evoked an increase in the production of the PGI2 metabolite 6-keto-PGF1␣, which was prevented by endothelial denudation or COX-1 Ϫ/Ϫ . Interestingly, COX-1 Ϫ/Ϫ was further found to abolish a force development that was sensitive to TP receptor antagonism and result in enhanced relaxation evoked by ACh following NO synthase inhibition. Also, in renal arteries the COX substrate arachidonic acid evoked a vasoconstrictor response, which was again abolished by COX-1 Ϫ/Ϫ . Meanwhile, nonselective COX inhibition did not show any effect in vessels from COX-1 Ϫ/Ϫ mice. Thus, in mouse renal arteries, high expression of TP receptors together with little functional involvement from the vasodilator PGI 2 receptors results in a potent vasoconstrictor effect evoked by PGI2. Also, our data imply that endogenous COX-1-mediated PGI2 synthesis leads to vasoconstrictor activity and this could be an integral part of endothelium-derived mechanisms in regulating local renal vascular function. arachidonic acid; TP receptors; contraction; IP receptors; vasodilation CYCLOOXYGENASE (COX), which exists in COX-1 and -2 isoforms, metabolizes arachidonic acid (AA) to produce various vasoactive prostanoids. Among them, prostacyclin [prostaglandin I 2 (PGI 2 )] is the major product generated in the endothelium, acting on the PGI 2 (IP) receptors on medial smooth muscle to mediate vasodilatation and protect vessels from the development of disease (4,25,33). Decreased production of endothelial PGI 2 synthesis has been suggested to cause increased incidence of cardiovascular events (8,12,40). On the other hand, studies also indicate that the endothelial COX-mediated metabolism generates vasoconstrictor products that act on thromboxane-prostanoid (TP) receptors to mediate vasoconstriction (9,14,16,28,30,32,43). Interestingly, PGI 2 can also activate smooth muscle TP receptors (11,21,22,36,38). This has been explained by an excessive production of PGI 2 and/or dysfunction of IP receptors found in conditions such as hypertension (11,36,38). Moreover, both TP and IP receptors may concomitantly modulate the vasomotor reaction to PGI 2 ; hence, in vessels with limited functional IP receptors the process of PGI 2 synthesis itself is suggeste...

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Vasoconstrictor prostanoids

Félétou

Huang

Vanhoutte

2010

Pflugers Arch - Eur J Physiol

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In cardiovascular diseases and during aging, endothelial dysfunction is due in part to the release of endothelium-derived contracting factors that counteract the vasodilator effect of the nitric oxide. Endothelium-dependent contractions involve the activation of endothelial cyclooxygenases and the release of various prostanoids, which activate thromboxane prostanoid (TP) receptors of the underlying vascular smooth muscle. The stimulation of TP receptors elicits not only the contraction and the proliferation of vascular smooth muscle cells but also diverse physiological/pathophysiological reactions, including platelet aggregation and activation of endothelial inflammatory responses. TP receptor antagonists curtail endothelial dysfunction in diseases such as hypertension and diabetes, are potent antithrombotic agents, and prevent vascular inflammation.

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Aldosterone induces endothelial dysfunction in resistance arteries from normotensive and hypertensive rats by increasing thromboxane A₂ and prostacyclin

Cited by 71 publications

References 26 publications

Mineralocorticoid Receptor Antagonist for Renal Protection

Mineralocorticoid Receptor Antagonist for Renal Protection

A vasoconstrictor role for cyclooxygenase-1-mediated prostacyclin synthesis in mouse renal arteries

Vasoconstrictor prostanoids

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Aldosterone induces endothelial dysfunction in resistance arteries from normotensive and hypertensive rats by increasing thromboxane A2 and prostacyclin

Cited by 71 publications

References 26 publications

Mineralocorticoid Receptor Antagonist for Renal Protection

Mineralocorticoid Receptor Antagonist for Renal Protection

A vasoconstrictor role for cyclooxygenase-1-mediated prostacyclin synthesis in mouse renal arteries

Vasoconstrictor prostanoids

Contact Info

Product

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Aldosterone induces endothelial dysfunction in resistance arteries from normotensive and hypertensive rats by increasing thromboxane A₂ and prostacyclin