Vasopressin-independent targeting of aquaporin-2 by selective E-prostanoid receptor agonists alleviates nephrogenic diabetes insipidus

Olesen, Emma Tina Bisgaard; Rützler, Michael; Moeller, Hanne B.; Praetorius, Helle A.; Fenton, Robert A.

doi:10.1073/pnas.1104691108

Cited by 113 publications

(93 citation statements)

References 32 publications

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“…16,18 EP2 has also been localized to mouse CCD cells, 14 the rabbit CCD, 33 and the human connecting tubule, 20 but kidney EP2 localization in mouse, rabbit, and human CDs is not consistently found. 13,14,21,22,33 EP2 is also expressed in renomedullary interstitial cells.…”

Section: Postobstructive Polyuriamentioning

confidence: 99%

Is There a Role for PGE2 in Urinary Concentration?

Olesen

Fenton

2013

Journal of the American Society of Nephrology

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Prostanoids are prominent, yet complex, components in the maintenance of body water homeostasis. Recent functional and molecular studies have revealed that the local lipid mediator PGE2 is involved both in water excretion and absorption. The biologic actions of PGE2 are exerted through four different G-protein-coupled receptors; designated EP1-4, which couple to separate intracellular signaling pathways. Here, we discuss new developments in our understanding of the actions of PGE2 that have been uncovered utilizing receptor specific agonists and antagonists, EP receptor and PG synthase knockout mice, polyuric animal models, and the new understanding of the molecular regulation of collecting duct water permeability. The role of PGE2 in urinary concentration comprises a variety of mechanisms, which are not fully understood and likely depend on which receptor is activated under a particular physiologic condition. EP3 and microsomal PG synthase type 1 play a role in decreasing collecting duct water permeability and increasing water excretion, whereas EP2 and EP4 can bypass vasopressin signaling and increase water reabsorption through two different intracellular signaling pathways. PGE2 has an intricate role in urinary concentration, and we now suggest how targeting specific prostanoid receptor signaling pathways could be exploited for the treatment of disorders in water balance. The neurohypophyseal hormone, vasopressin (VP), is a major regulator of renal water excretion, predominantly through the seven trans-membrane receptor (7TMR) V2R. It binds to Gas, inducing the cAMP second messenger system, resulting in increased NaCl absorption by the thick ascending limb and increased urea transport in the inner medullary collecting ducts (IMCDs). [1][2][3] In addition, VP induces accumulation of the water channel aquaporin-2 (AQP2) in the rate-limiting apical plasma membrane of collecting duct (CD) principal cells, 4 a process that involves a diverse range of post-translational modifications including phosphorylation of AQP2. 5 Thus, VP increases the osmotic gradient for water transport and the water permeability (Pf) of the CD simultaneously.In addition to systemic hormones, local regulatory factors play a role in the CD, of which PGE2 (Figure 1) is the focus of this review. 6-9 PGE2 has a diverse range of biologic actions elicited by four different 7TMRs. The renal localization of EP receptors and intracellular signaling pathways are diverse (Table 1). Here, we propose that urinary concentration does not rely exclusively on fluctuations in plasma VP concentrations, but that the locally derived lipid mediator, PGE2, plays an important role in regulating water excretion. PGE2 IN THE MODULATION OF URINARY CONCENTRATING MECHANISMSThe ability of PGE2 to modulate the effects of VP in the CD has been described in a range of experimental studies and discussed in previous reviews. [36][37][38][39] The present focus is on understanding the mechanisms for this effect, and on recent in vivo studies elucidating the role of P...

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Section: Postobstructive Polyuriamentioning

confidence: 99%

Is There a Role for PGE2 in Urinary Concentration?

Olesen

Fenton

2013

Journal of the American Society of Nephrology

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“…This is a potential mechanism by which prostaglandin inhibitors such as nonsteroidal anti-inflammatory agents may cause fluid retention. Recent studies done in Madin-Darby canine kidney cells show that AQP-2 phosphorylation and apical insertion are increased by prostaglandin EP2 and EP4 receptors activation [23]. It has also been shown in rats that butaprost, a EP2 agonist can increase urinary concentration in rats with the V2R blocked.…”

Section: Introductionmentioning

confidence: 99%

Diabetes Insipidus: A Review

Shapiro¹

2013

J Diabetes Metab

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“…Conversely, inhibition of prostaglandine synthesis by indomethacine enhances the effect of vasopressin [31,32]. Recently, data for the role of PGE2 in urinary concentration were published that conflict with the earlier results of an antagonism between PGE2 and vasopressin [33]: these data show a vasopressin-independent direct increase in cAMP and consequent Aqp2 phosphorylation and membrane insertion after treatment with PGE2 or related agonists for the E-prostanoid receptors EP2 or EP4. Indeed, rats treated with a blocker of Avpr2 develop a pharmacologically induced NDI and the phenotype could be significantly alleviated by treatment with an EP2 agonist [33].…”

Section: Prostaglandinsmentioning

confidence: 92%

“…The recent data on AVPR2-independent activation by agonists for the EP2 and EP4 receptors raises the intriguing possibility of a new therapeutic pathway for patients with X-linked NDI [33]. However, at this point it is unclear how to resolve the contradiction between giving prostaglandins to reduce urine output, when the blockade of their synthesis by indomethacine has actually proven clinical efficacy.…”

Section: Pge Agonistsmentioning

confidence: 99%

Urinary concentration: different ways to open and close the tap

Böckenhauer

Bichet

2013

Pediatr Nephrol

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Nephrogenic diabetes insipidus (NDI) provides an excellent model for the benefits and insights that can be gained from studying rare diseases. The discovery of underlying genes identified key molecules involved in urinary concentration, including the type 2 vasopressin receptor AVPR2 and the water channel AQP2, which constitute obvious pharmacologic targets. Subsequently developed drugs targeting AVPR2 not only provide potential benefit to some patients with NDI, but are now used for much more common clinical applications as diverse as nocturnal enuresis and heart failure. Yet, the story is still evolving:clinical observations and animal experiments continue to discover new ways to affect urinary concentration. These novel pathways can potentially be exploited for therapeutic gain. Here we review the (patho)physiology of water homoeostasis, the current status of clinical management and potential new treatments.3

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Vasopressin-independent targeting of aquaporin-2 by selective E-prostanoid receptor agonists alleviates nephrogenic diabetes insipidus

Cited by 113 publications

References 32 publications

Is There a Role for PGE2 in Urinary Concentration?

Is There a Role for PGE2 in Urinary Concentration?

Diabetes Insipidus: A Review

Urinary concentration: different ways to open and close the tap

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