Efficacy and Safety of DA-8010, a Novel M3 Antagonist, in Patients With Overactive Bladder: A Randomized, Double-Blind Phase 2 Study

Hee Seo Son; Cheol Young Oh; Myung-Soo Choo; Hyeong Gon Kim; Joon Chul Kim; Kyu-Sung Lee; Dong Gil Shin; Sung Yong Cho; Seong Jin Jeong; Ju Tae Seo; Hana Yoon; Hong Sang Moon; Jang Hwan Kim

doi:10.5213/inj.2142382.191

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Efficacy and Safety of DA-8010, a Novel M3 Antagonist, in Patients With Overactive Bladder: A Randomized, Double-Blind Phase 2 Study

Authors: Hee Seo Son ; Cheol Young Oh ; Myung-Soo Choo ; Hyeong Gon Kim ; Joon Chul Kim ; Kyu-Sung Lee ; Dong Gil Shin ; Sung Yong Cho ; Seong Jin Jeong ; Ju Tae Seo ; Hana Yoon ; Hong Sang Moon ; Jang Hwan Kim

Citation: INTERNATIONAL NEUROUROLOGY JOURNAL(대한배뇨장애요실금학회지), Vol.26(2) : 119-128, 2022-06

Journal Title: INTERNATIONAL NEUROUROLOGY JOURNAL(대한배뇨장애요실금학회지)

ISSN: 2093-4777

Issue Date: 2022-06

Keywords: DA-8010 ; Muscarinic antagonists ; Overactive ; Receptor, Muscarinic M3 ; Urinary bladder

Abstract: Purpose: DA-8010 is a novel muscarinic M3 receptor antagonist with significant selectivity for bladder over salivary gland in preclinical studies. We evaluated the clinical efficacy and safety of DA-8010 in overactive bladder (OAB) patients.

Methods: This phase 2, randomized, double-blind, parallel-group, active reference- and placebo-controlled trial was conducted at 12 centers in South Korea (NCT03566134). Patients aged ≥19 years with OAB symptoms for ≥3 months were enrolled. Three hundred six patients (30.07% male) were randomized to 12 weeks of treatment among 4 groups; 2 experimental groups (DA-8010 2.5 or 5 mg), an active reference group (solifenacin 5 mg), and a placebo group. The change from the baseline of (=∆) 24-hour frequency at 12 weeks (primary endpoint), episodes of urgency, overall/urgency urinary incontinence, average/ maximum voided volume, nocturia, and patients' subjective responses were analyzed.

Results: In the full analysis set, the mean (standard deviation) [median] values for ∆ 24-hour frequency at 12 weeks were -1.01 (2.44) [-1.33] for placebo, -1.22 (2.05) [-1.33] for DA-8010 2.5 mg, and -1.67 (2.25) [-1.67] for DA-8010 5 mg; DA-8010 5 mg showed a significant decrease compared with placebo (P=0.0413). At 4 and 8 weeks, both DA-8010 2.5 mg (P=0.0391 at 4 weeks, P=0.0335 at 8 weeks) and DA-8010 5 mg (P=0.0001 at 4 weeks, P=0.0210 at 8 weeks) showed significant decrease in ∆ 24-hour frequency compared with placebo. DA-8010 5 mg achieved a significant decrease in ∆ number of urgency episodes, compared with placebo at 4 (P=0.0278) and 8 (P=0.0092) weeks. Adverse drug reactions (ADRs) were observed in 3.95% of placebo, 6.67% of DA-8010 2.5 mg, 18.42% of DA-8010 5 mg, and 17.33% of solifenacin 5 mg groups. No serious ADRs were observed in any patient.

Conclusion: Both DA-8010 2.5 mg and 5 mg showed therapeutic efficacy for OAB without serious ADRs. Therefore, both dosages of DA-8010 can advance to a subsequent large-scale phase 3 trial.