Efficacy and safety of epaminurad, a potent hURAT1 inhibitor, in patients with gout: a randomized, placebo-controlled, dose-finding study

IF 4.9 2区医学 Q1 Medicine

Arthritis Research & Therapy Pub Date : 2025-05-26 DOI:10.1186/s13075-025-03577-w

Jae-Bum Jun, Hye-Soon Lee, Sang-Hyon Kim, Seung-Geun Lee, Doo-Ho Lim, Jinhyun Kim, Yong-Beom Park, Mie Jin Lim, Seung-Jae Hong, Hyo-Jin Choi, Shin-Seok Lee, Hyun Ah Kim, Jiwon Hwang, Chang-Hee Suh, Seungwoo Han, Jung-Yoon Choe, Wan-Hee Yoo, Jung Soo Song

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引用次数: 0

Abstract

Gout is the most common inflammatory arthritis. Current urate-lowering therapies have limitations, such as adverse drug reactions or limited efficacy. Epaminurad is a novel selective human urate transporter 1 (hURAT1) inhibitor that has been shown to reduce serum urate (sUA) levels in healthy volunteers and patients with gout. The aims of the current study were to evaluate the urate-lowering efficacy and safety of epaminurad compared with placebo in patients with gout, and to determine the optimal dose. This multicenter, randomized, double-blind, placebo-controlled, dose-finding phase 2b clinical trial, which incorporated a standard-treatment reference arm, enrolled patients aged 19–70 years with gout and sUA level ≥ 0.42 mmol/L. Participants received gout prophylaxis and followed therapeutic lifestyle changes, and were randomized to receive epaminurad 3 mg, 6 mg or 9 mg, or febuxostat 80 mg, or matching placebo, once daily for 12 weeks. The primary efficacy endpoint was the proportion of patients with sUA level < 0.36 mmol/L at week 4 after initiation of study treatment. Statistical comparisons were performed between the epaminurad and placebo groups. Overall, 169 patients received study medication (99.40% male, mean ± SD age 48.26 ± 13.15 years, sUA level 0.53 ± 0.09 mmol/L). Mean adherence to treatment was > 90% in all groups. The proportion of patients with sUA < 0.36 mmol/L at week 4 was significantly higher in each epaminurad group (9 mg, 88.89%; 6 mg, 71.79%; 3 mg, 54.05%) compared with placebo (0.00%) (all p < 0.0001). The response rate in the febuxostat group was 84.21%. The proportion of patients who achieved sUA < 0.30 mmol/L, and mean percent and absolute change in sUA, were also significantly greater in all epaminurad groups versus placebo at week 4. Outcomes were consistent at weeks 8 and 12. The adverse event rate did not differ between epaminurad groups and placebo, and most events were mild. There were no significant differences in mean serum creatinine levels or liver function parameters between the epaminurad groups and placebo. Epaminurad was effective at reducing sUA levels in patients with gout. The study also confirmed the safety and tolerability profile during 12 weeks of treatment. ClinicalTrials.gov NCT04804111 (registered on 15 November 2020).

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epaminurad（一种强效hURAT1抑制剂）在痛风患者中的疗效和安全性：一项随机、安慰剂对照、剂量发现研究

痛风是最常见的炎症性关节炎。目前的降尿酸疗法有局限性，如药物不良反应或疗效有限。Epaminurad是一种新型的选择性人尿酸转运蛋白1 （hURAT1）抑制剂，已被证明可以降低健康志愿者和痛风患者的血清尿酸（sUA）水平。本研究的目的是评估epaminurad与安慰剂相比在痛风患者中降低尿酸盐的疗效和安全性，并确定最佳剂量。这项多中心、随机、双盲、安慰剂对照、剂量寻找的2b期临床试验纳入了一个标准治疗参考组，纳入了年龄19-70岁痛风且sUA水平≥0.42 mmol/L的患者。参与者接受痛风预防，并遵循治疗性生活方式的改变，并随机接受依米努拉德3毫克，6毫克或9毫克，或非布司他80毫克，或匹配安慰剂，每天一次，持续12周。主要疗效终点为各组中sUA水平为90%的患者比例。各组患者第4周sUA < 0.36 mmol/L的比例显著高于依米努拉德组(9 mg, 88.89%；6 mg，占71.79%；3 mg, 54.05%)与安慰剂（0.00%）相比（均p < 0.0001）。非布司他组有效率为84.21%。在第4周，所有依米努拉德组达到sUA < 0.30 mmol/L的患者比例，以及sUA的平均百分比和绝对变化也显著高于安慰剂组。结果在第8周和第12周一致。依米努拉德组和安慰剂组的不良事件发生率没有差异，大多数不良事件是轻微的。在依米努拉德组和安慰剂组之间，平均血清肌酐水平或肝功能参数没有显著差异。Epaminurad能有效降低痛风患者的sUA水平。该研究还证实了12周治疗期间的安全性和耐受性。ClinicalTrials.gov NCT04804111（注册于2020年11月15日）。

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来源期刊

Arthritis Research & Therapy RHEUMATOLOGY-

CiteScore

8.60

自引率

2.00%

发文量

261

审稿时长

14 weeks

期刊介绍： Established in 1999, Arthritis Research and Therapy is an international, open access, peer-reviewed journal, publishing original articles in the area of musculoskeletal research and therapy as well as, reviews, commentaries and reports. A major focus of the journal is on the immunologic processes leading to inflammation, damage and repair as they relate to autoimmune rheumatic and musculoskeletal conditions, and which inform the translation of this knowledge into advances in clinical care. Original basic, translational and clinical research is considered for publication along with results of early and late phase therapeutic trials, especially as they pertain to the underpinning science that informs clinical observations in interventional studies.