Bladder selectivity of the novel β3-agonist ritobegron (KUC-7483) explored by in vitro and in vivo studies in the rat

Maruyama, Itaru; Goi, Yoshiaki; Tatemichi, Satoshi; Maruyama, Kazuyasu; Hoyano, Yuji; Yamazaki, Yoshinobu; Kusama, Hiroshi

doi:10.1007/s00210-012-0755-x

Cited by 26 publications

(19 citation statements)

References 17 publications

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“…In two series of experiments performed with similar protocols but with bladder strips from Japanese and German patients, we have demonstrated that KUC-7322 is 0.7-1.0 log units less potent than the reference agonist isoproterenol but has a comparable efficacy. These findings are in line with findings for rat detrusor relaxation, where KUC-7322 also was slightly less potent but similarly efficacious as isoproterenol (Maruyama et al 2012). In rats, these in vitro findings translated into a dosedependent reduction of intravesicular pressure in anesthetized animals in vivo by ritobegron, the prodrug of KUC-7322 (Maruyama et al 2012).…”

Section: Detrusor Relaxation Findingssupporting

confidence: 87%

“…KUC-7322 is the active metabolite of ritobegron (also known as and was reported to be 301-and 32-fold selective for β3-AR over β1-AR and β2-AR for stimulation of cAMP formation by cloned human receptor subtypes; a similar selectivity profile was obtained by comparing its potency for relaxation of rat bladder as compared to rat atrium and myometrium (Maruyama et al 2012). In two series of experiments performed with similar protocols but with bladder strips from Japanese and German patients, we have demonstrated that KUC-7322 is 0.7-1.0 log units less potent than the reference agonist isoproterenol but has a comparable efficacy.…”

Section: Detrusor Relaxation Findingsmentioning

confidence: 88%

“…Ritobegron (also known as KUC-7483) is a novel compound developed in the search for a promising drug for overactive bladder syndromes carried out by Kissei Pharmaceutical Co. Ltd. After oral administration, KUC-7483 is rapidly converted to KUC-7322, a selective β3-AR agonist (Maruyama et al 2012). It was recently reported (a) that KUC-7322 has selective agonistic activity for the human β3-AR and a potent relaxing effect on the isolated rat bladder via stimulation of β3-AR and (b) that it decreases intravesical pressure in rats with minimal effects on the cardiovascular system (Maruyama et al 2012). In the present study, we characterized the β-AR subtype mediating human detrusor relaxation based on agonists and antagonists and determined the ability of KUC-7322 to cause relaxation and to prevent contraction of isolated human detrusor.…”

Section: Introductionmentioning

confidence: 99%

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Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Igawa

Schneider

Yamazaki

et al. 2012

Naunyn-Schmiedeberg's Arch Pharmacol

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This study aimed to characterize the β-adrenoceptor (β-AR) subtype mediating relaxation of isolated human bladder strips and to explore relaxation by the novel β3-AR-selective agonist KUC-7322 for its relaxant effect on the human isolated detrusor and for its effect on the carbachol (CCh)-induced contractile response. In two parallel studies, relaxation of isolated human bladder strips was tested for the β-AR agonists isoproterenol, clenbuterol, BRL 37344, and KUC-7322. For the isoproterenol and KUC-7322 responses, antagonism by CGP 20712A, ICI 118551, and SR59230A was determined. The potency and efficacy of the reference agonists for detrusor relaxation was in line with their known β3-AR activity. KUC-7322 relative to isoproterenol was a full agonist with a pEC(50) of 5.95 ± 0.09 and 5.92 ± 0.11 in the two studies. SR59230A exhibited antagonism of the expected potency against isoproterenol (apparent pK (B) 7.2) but not against KUC-7322. Neither isoproterenol nor KUC-7322 nor forskolin significantly attenuated CCh-induced contraction. These results suggest that KUC-7322 displays full agonistic activity in relaxing the human detrusor without inhibiting the contraction induced by cholinergic stimulation. These characteristics, if proven in vivo, may be beneficial for the treatment of overactive bladder, as increased bladder capacity with a negligible effect on voiding contractions may be anticipated.

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Section: Detrusor Relaxation Findingssupporting

confidence: 87%

Section: Detrusor Relaxation Findingsmentioning

confidence: 88%

Section: Introductionmentioning

confidence: 99%

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Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Igawa

Schneider

Yamazaki

et al. 2012

Naunyn-Schmiedeberg's Arch Pharmacol

Self Cite

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“…Before this study, we were apprehensive that an increase in exposure of KUC-7322 might affect ECG parameters such as the heart rate and QT interval because KUC-7322 is a weak b 1 -and b 2-adrenoceptors agonist, even though it is highly selective for the b 3 -adrenoceptor; the selectivity of KUC-7322 for b 1 -and b 2-adrenoceptors is 1/301 and 1/32, respectively, of that for the b 3 -adrenoceptor. 6 Although an increase in exposure and a decrease in clearance were observed following coadministration of probenecid, there were no clinically significant abnormal ECG changes in this study. Furthermore, there were no obvious differences in subjective/objective findings, vital signs (blood pressure, pulse rate, and temperature), physical examinations (body weight), and clinical laboratory values (hematology, blood chemistry, and urinalysis) between ritobegron alone and ritobegron in combination with probenecid.…”

Section: Discussioncontrasting

confidence: 47%

“…To measure the KUC-7322 concentrations, blood samples (2 mL per time) were collected in vacuum blood collection tubes containing ethylenediaminetetraacetic acid disodium salt, sodium fluoride, and heparin at the following times after administration of ritobegron: 0.25, 0.5, 1, 1.5, 2, 3, 4,6,8,12,14,24,36, and 48 hours. Blood samples were centrifuged (3000 rpm) at 4˚C for 10 minutes and separated.…”

Section: Sample Collectionmentioning

confidence: 99%

Investigation of Drug–Drug Interactions Between Ritobegron, a Selective β₃‐Adrenoceptor Agonist, With Probenecid in Healthy Men

Abe

Nakano

Kanazawa

et al. 2015

Clinical Pharm in Drug Dev

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We evaluated the effects of probenecid, a potent organic anion transporter 1 (OAT1) and OAT3 inhibitor, on the pharmacokinetics and safety of ritobegron, a selective β3 -adrenoceptor agonist, in healthy men. Twelve healthy men were administered a single oral dose of ritobegron (20 mg) alone or in combination with probenecid 2 hours before administration of ritobegron. In the combination sequence, additional doses of probenecid were administered 4 and 10 hours after the administration of ritobegron. Probenecid increased the Cmax of KUC-7322, an active form of ritobegron, and the AUC0-48 h by 1.39 and 2.93 times, respectively. Probenecid prolonged the t1/2 of KUC-7322 from 1.6 to 3.4 hours and decreased the renal clearance and cumulative fraction of KUC-7322 excreted in urine from 18.5 to 4.9 L/h and from 64.7% to 49.7%, respectively. Coadministration of probenecid did not influence adverse events, blood pressure, pulse rate, or heart rate relative to ritobegron alone. Although probenecid inhibited renal tubule secretion of KUC-7322 via OAT3 and increased KUC-7322 exposure, it did not influence adverse effects or vital signs. Therefore, clinically significant drug-drug interactions are unlikely to occur when probenecid is administered in combination with OAT3 inhibitors or substrates.

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Pharmacophore‐guided Virtual Screening to Identify New β₃‐adrenergic Receptor Agonists

Ujiantari

Ham

Nagiri

et al. 2022

Molecular Informatics

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The β3‐adrenergic receptor (β3‐AR) is found in several tissues such as adipose tissue and urinary bladder. It is a therapeutic target because it plays a role in thermogenesis, lipolysis, and bladder relaxation. Two β3‐AR agonists are used clinically: mirabegron 1 and vibegron 2, which are indicated for overactive bladder syndrome. However, these drugs show adverse effects, including increased blood pressure in mirabegron patients. Hence, new β3‐AR agonists are needed as starting points for drug development. Previous pharmacophore modeling studies of the β3‐AR did not involve experimental in vitro validation. Therefore, this study aimed to conduct prospective virtual screening and confirm the biological activity of virtual hits. Ligand‐based pharmacophore modeling was performed since no 3D structure of human β3‐AR is yet available. A dataset consisting of β3‐AR agonists was prepared to build and validate the pharmacophore models. The best model was employed for prospective virtual screening, followed by physicochemical property filtering and a docking evaluation. To confirm the activity of the virtual hits, an in vitro assay was conducted, measuring cAMP levels at the cloned β3‐AR. Out of 35 tested compounds, 4 compounds were active in CHO−K1 cells expressing the human β3‐AR, and 8 compounds were active in CHO−K1 cells expressing the mouse β3‐AR.

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Bladder selectivity of the novel β3-agonist ritobegron (KUC-7483) explored by in vitro and in vivo studies in the rat

Cited by 26 publications

References 17 publications

Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Investigation of Drug–Drug Interactions Between Ritobegron, a Selective β₃‐Adrenoceptor Agonist, With Probenecid in Healthy Men

Pharmacophore‐guided Virtual Screening to Identify New β₃‐adrenergic Receptor Agonists

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Bladder selectivity of the novel β3-agonist ritobegron (KUC-7483) explored by in vitro and in vivo studies in the rat

Cited by 26 publications

References 17 publications

Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Functional investigation of β-adrenoceptors in human isolated detrusor focusing on the novel selective β3-adrenoceptor agonist KUC-7322

Investigation of Drug–Drug Interactions Between Ritobegron, a Selective β3‐Adrenoceptor Agonist, With Probenecid in Healthy Men

Pharmacophore‐guided Virtual Screening to Identify New β3‐adrenergic Receptor Agonists

Contact Info

Product

Resources

About

Investigation of Drug–Drug Interactions Between Ritobegron, a Selective β₃‐Adrenoceptor Agonist, With Probenecid in Healthy Men

Pharmacophore‐guided Virtual Screening to Identify New β₃‐adrenergic Receptor Agonists