Reversal of postischemic acute renal failure with a selective endothelinA receptor antagonist in the rat.

Gellai, Miklos; Jugus, M; Fletcher, Tracey; DeWolf, Robin; Nambi, Ponnal

doi:10.1172/jci117046

Cited by 199 publications

(97 citation statements)

References 26 publications

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“…Recent studies indicated that the ET-1/ET A receptor system may be an important mediator in the pathogenesis of postischemic acute renal failure, based on findings that ET-1 mRNA expression is markedly enhanced in the postischemic kidney 32 and that a selective ET A receptor antagonist prevents postischemic renal damage, such as decreases in renal blood flow and glomerular filtration rate, and tubular dysfunction. 11,12 Further investigations are required to clarify whether the ABT-627-induced improvement in vascular hypertrophy and renal damage in DOCA-salt hypertension is independent of its antihypertensive activity.…”

Section: Matsumura Et Al February 1999 763mentioning

confidence: 99%

“…8,9 We noted the ameliorating effect of FR 139317, an ET A -selective receptor antagonist, on decreased renal function of DOCAsalt hypertensive rats. 10 On the other hand, both ET A -selective and nonselective ET A /ET B receptor antagonists have been reported to prevent various cardiovascular diseases, such as acute ischemic renal failure [11][12][13] and chronic heart failure, 14,15 in animal models. Thus, it remains obscure as to whether blockade of the ET B receptor is beneficial for the treatment of subjects with cardiovascular diseases.…”

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confidence: 99%

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Different Contributions of Endothelin-A and Endothelin-B Receptors in the Pathogenesis of Deoxycorticosterone Acetate–Salt–Induced Hypertension in Rats

et al. 1999

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Abstract-We investigated the involvement of actions mediated by endothelin-A (ET A ) and endothelin-B (ET B ) receptors in the pathogenesis of deoxycorticosterone acetate (DOCA)-salt-induced hypertension in rats. Two weeks after the start of DOCA-salt treatment, rats were given ABT-627 (10 [mg/kg]/d), a selective ET A receptor antagonist; A-192621 (30 [mg/kg]/d), a selective ET B receptor antagonist; or their vehicle for 2 weeks. Uninephrectomized rats without DOCA-salt treatment served as controls. Treatment with DOCA and salt for 2 weeks led to a mild but significant hypertension; in vehicle-treated DOCA-salt rats, systolic blood pressure increased markedly after 3 to 4 weeks. Daily administration of ABT-627 for 2 weeks almost abolished any further increases in blood pressure, whereas A-192621 did not affect the development of DOCA-salt-induced hypertension. When the degree of vascular hypertrophy of the aorta was histochemically evaluated at 4 weeks, there were significant increases in wall thickness, wall area, and wall-to-lumen ratio in vehicle-treated DOCA-salt rats compared with uninephrectomized control rats. The development of vascular hypertrophy was markedly suppressed by ABT-627. In contrast, treatment with A-192621 significantly exaggerated these vascular changes. In vehicle-treated DOCA-salt rats, renal blood flow and creatinine clearance decreased, and urinary excretion of protein, blood urea nitrogen, fractional excretion of sodium, and urinary N-acetyl-␤-glucosaminidase activity increased. Such damage was overcome by treatment with ABT-627 but not with A-192621; indeed, the latter agent led to worsening of the renal dysfunction. Histopathologic examination of the kidney in vehicle-treated DOCA-salt rats revealed tubular dilatation and atrophy as well as thickening of small arteries. Such damage was reduced in animals given ABT-627, whereas more severe histopathologic changes were observed in A-192621-treated animals. These results strongly support the view that ET A receptor-mediated action plays an important role in the pathogenesis of DOCA-salt-induced hypertension. On the other hand, it seems likely that the ET B receptor-mediated action protects against vascular and renal injuries in this model of hypertension. A selective ET A receptor antagonist is likely to be useful for treatment of subjects with mineralocorticoid-dependent hypertension, whereas ET B -selective antagonism alone is detrimental to such cases. (Hypertension. 1999;33:759-765.)Key Words: receptors, endothelin Ⅲ hypertension, DOCA-salt Ⅲ renal function Ⅲ vascular hypertrophy T here is accumulating evidence indicating that endothelin-1 (ET-1) plays an important role in the development and/or maintenance of hypertension in animal models such as the deoxycorticosterone acetate (DOCA)-salt-induced hypertensive rat 1-6 and Dahl salt-sensitive rat. 7,8 This view is based on findings indicating that acute administration of an endothelin-A (ET A )-selective receptor antagonist or nonselective ET A /ET B receptor antagonist to DOCAsal...

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Section: Matsumura Et Al February 1999 763mentioning

confidence: 99%

mentioning

confidence: 99%

Different Contributions of Endothelin-A and Endothelin-B Receptors in the Pathogenesis of Deoxycorticosterone Acetate–Salt–Induced Hypertension in Rats

et al. 1999

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“…To date, the results indicate that ischemia-induced ARF is attenuated by the infusion of anti-endothelin antibody or a receptor antagonist during ischemia or the early phase of reperfusion. In a recent study, however, BQ-123 infused 24 hr after the onset of ischemia was shown to effectively reverse renal damage in rats with ARF, clearly indicating that an ETA antagonist is efficacious even in the treatment of established ARF (182). Furthermore, since the negative actions of endothelin-1 on renal function in ARF are more marked during the maintenance phase than the initial phase after ischemia, endothelin receptor antagonists appear to be more effective in reversing than in preventing renal impairment (183,184).…”

Section: V-3 Acute Renal Failurementioning

confidence: 96%

Molecular Pharmacology and Pathophysiological Significance of Endothelin

Goto

Hama

Kasuya

1996

Japanese Journal of Pharmacology

159

108

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ABSTRACT-Since the discovery of the most potent vasoconstrictor peptide, endothelin, in 1988, explosive investigations have rapidly clarified much of the basic pharmacological, biochemical and molecular biological features of endothelin, including the presence and structure of isopeptides and their genes (endothelin-1, -2 and -3), regulation of gene expression, intracellular processing, specific endothelia converting enzyme (ECE), receptor subtypes (ETA and ETB), intracellular signal transduction following receptor activation, etc. ECE was recently cloned, and its structure was shown to be a single transmembrane protein with a short intracellular N-terminal and a long extracellular C-terminal that contains the catalytic domain and numerous N-glycosylation sites. In addition to acute contractile or secretory actions, endothelin has been shown to exert long-term proliferative actions on many cell types. In this case, intracellular signal transduction appears to converge to activation of mitogen-activated protein kinase. As a recent dramatic advance, a number of non-peptide and orally active receptor antagonists have been developed. They, as well as current peptide antagonists, markedly accelerated the pace of investigations into the true pathophysiological roles of endogenous endothelin-1 in mature animals; e.g., hypertension, pulmonary hypertension, acute renal failure, cerebral vasospasm, vascular thickening, cardiac hypertrophy, chronic heart failure, etc. Thus, the interference with the endothelin pathway by either ECE-inhibition or receptor blockade may

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“…At least five studies have shown that ET-1 receptor blockade either conferred no functional protection, or worsened post-ischemic AKI [36][37][38][39][40]. In a more recent ischemia-reperfusion model in mice undergoing unilateral ischemia without contralateral nephrectomy, an increase in intrarenal ET-1 production was observed, along with increased expression of the ET A receptor and evidence of ET-1 gene activation alongside progressive histological changes and a 40% loss of renal mass [41].…”

Section: Endothelin-1mentioning

confidence: 99%

Long-term Sequelae from Acute Kidney Injury: Potential Mechanisms for the Observed Poor Renal Outcomes

Varrier

Forni

Ostermann

2015

Annual Update in Intensive Care and Emergency Medicine

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Reversal of postischemic acute renal failure with a selective endothelinA receptor antagonist in the rat.

Cited by 199 publications

References 26 publications

Different Contributions of Endothelin-A and Endothelin-B Receptors in the Pathogenesis of Deoxycorticosterone Acetate–Salt–Induced Hypertension in Rats

Different Contributions of Endothelin-A and Endothelin-B Receptors in the Pathogenesis of Deoxycorticosterone Acetate–Salt–Induced Hypertension in Rats

Molecular Pharmacology and Pathophysiological Significance of Endothelin

Long-term Sequelae from Acute Kidney Injury: Potential Mechanisms for the Observed Poor Renal Outcomes

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