Effect of Selective Prostaglandin <scp>E<sub>2</sub> EP2</scp> Receptor Agonist <scp>CP</scp>‐533,536 on Voiding Efficiency in Rats with Midodrine‐Induced Functional Urethral Obstruction

Kurihara, Ryoko; Imazumi, Katsunori; Takamatsu, Hajime; Ishizu, Kenichiro; Yoshino, Taiji; Masuda, Noriyuki

doi:10.1111/luts.12080

Cited by 3 publications

(4 citation statements)

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“…CP‐533,536 dose‐dependently decreased perfusion pressure, but had no effect on maximum voiding pressure, intercontraction interval, or intravesical threshold pressure. In conscious rats, where midodrine markedly increased residual volume, and reduced VE, CP‐533,536 dose‐dependently counteracted these effects …”

Section: Methodsmentioning

confidence: 97%

“…In spinal cord injured (SCI) rats, Wada et al found that the PGE2‐induced activation of EP1 receptors in the spinal cord contributes to the initiation of bladder over activity, and concluded that the EP1 receptor could be a therapeutic target for the treatment of neurogenic DO due to SCI. The selective EP2 receptor agonist, CP‐533,536, was tested on voiding efficiency (VE) in anesthetised rats with functional urethral obstruction, induced by midodrine . CP‐533,536 dose‐dependently decreased perfusion pressure, but had no effect on maximum voiding pressure, intercontraction interval, or intravesical threshold pressure.…”

Section: Methodsmentioning

confidence: 99%

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Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Andersson

Fry

Panicker

et al. 2018

Neurourology and Urodynamics

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Section: Methodsmentioning

confidence: 97%

Section: Methodsmentioning

confidence: 99%

Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Andersson

Fry

Panicker

et al. 2018

Neurourology and Urodynamics

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“…All surgical procedures and measurement of micturition parameters via cystometry were performed based on a previously described method. 19,20 Briefly, a catheter (PE-160; Becton, Dickinson & Co., Franklin Lakes, NJ, USA) for saline infusion into the bladder and collection of residual urine after voiding was inserted into the bladder and connected to a pressure transducer (DX-100; Nihon Kohden, Tokyo, Japan) and infusion pump (TE-331S, STC-528; Terumo Co., Tokyo, Japan) via a three-way tap. Each rat was placed in a Ballman's cage (Natsume Seisakusho Co., Ltd., Tokyo, Japan).…”

Section: Evaluation Of Voiding Function In Rats With Voiding Dysfunct...mentioning

confidence: 99%

“…We hypothesize that a considerable number of patients suffering from lower urinary tract symptoms with various possible pathophysiologies including aging 30 have such a condition but are left underdiagnosed because of a lack of clear urodynamically confirmed DU or BOO. 31 We pharmacologically reproduced this condition by administering a combination of atropine and midodrine at doses lower than those used in previous studies, 19,32,33 and applying the experimental methods we used previously 19,20 (Figure 3). In this model, we used the effects of distigmine at 0.003 mg/kg iv as a benchmark because it significantly enhanced the PNS-induced elevation of IVP (Figure 2C) at the plasma concentration similar to that of the clinically efficacious dose (15 mg/man/d) 34,35 (data not shown).…”

Section: Number Of Stoolsmentioning

confidence: 99%

Muscarinic M₃ positive allosteric modulator ASP8302 enhances bladder contraction and improves voiding dysfunction in rats

Okimoto

Ino

Ishizu

et al. 2022

LUTS

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Objectives Muscarinic M3 (M3) receptors mediate cholinergic smooth muscle contraction of the bladder. Current drugs targeting bladder M3 receptors for micturition disorders have a risk of cholinergic side effects due to excessive receptor activation and insufficient selectivity. We investigated the effect of ASP8302, a novel positive allosteric modulator (PAM) of M3 receptors, on bladder function in rats. Methods Modulation of carbachol‐induced increases in intracellular Ca2+ was assessed in cells expressing rat muscarinic receptors. Potentiation of bladder contractions was evaluated using isolated rat bladder strips and by measuring intravesical pressure in anesthetized rats. Conscious cystometry was performed to investigate the effects on residual urine volume and voiding efficiency in rat voiding dysfunction models induced by the α1‐adrenoceptor agonist midodrine and muscarinic receptor antagonist atropine, and bladder outlet obstruction. To assess potential side effects, the number of stools and tracheal insufflation pressure were measured in conscious and anesthetized rats, respectively. Results ASP8302 demonstrated PAM effects on the rat M3 receptor in cell assays, and augmented cholinergic bladder contractions both in vivo and in vitro. ASP8302 improved voiding efficiency and reduced residual urine volume in two voiding dysfunction models as effectively as distigmine bromide, but unlike distigmine bromide did not affect the number of stools or tracheal insufflation pressure. Conclusions Our results in rats indicate that ASP8302 improves voiding dysfunction by potentiating bladder contraction with fewer effects on cholinergic responses in other organs, and suggest a potential advantage over current cholinomimetic drugs for treating micturition disorders caused by insufficient bladder contraction.

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ASP6432, a type 1 lysophosphatidic acid receptor antagonist, reduces urethral function during urine voiding and improves voiding dysfunction

Sakamoto

Noguchi

Imazumi

et al. 2019

European Journal of Pharmacology

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Effect of Selective Prostaglandin E₂ EP2 Receptor Agonist CP‐533,536 on Voiding Efficiency in Rats with Midodrine‐Induced Functional Urethral Obstruction

Cited by 3 publications

References 27 publications

Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Muscarinic M₃ positive allosteric modulator ASP8302 enhances bladder contraction and improves voiding dysfunction in rats

ASP6432, a type 1 lysophosphatidic acid receptor antagonist, reduces urethral function during urine voiding and improves voiding dysfunction

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Effect of Selective Prostaglandin E2 EP2 Receptor Agonist CP‐533,536 on Voiding Efficiency in Rats with Midodrine‐Induced Functional Urethral Obstruction

Cited by 3 publications

References 27 publications

Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Which molecular targets do we need to focus on to improve lower urinary tract dysfunction? ICI‐RS 2017

Muscarinic M3 positive allosteric modulator ASP8302 enhances bladder contraction and improves voiding dysfunction in rats

ASP6432, a type 1 lysophosphatidic acid receptor antagonist, reduces urethral function during urine voiding and improves voiding dysfunction

Contact Info

Product

Resources

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Effect of Selective Prostaglandin E₂ EP2 Receptor Agonist CP‐533,536 on Voiding Efficiency in Rats with Midodrine‐Induced Functional Urethral Obstruction

Muscarinic M₃ positive allosteric modulator ASP8302 enhances bladder contraction and improves voiding dysfunction in rats