Klück Viola, Jansen Tim L Th A, Janssen Matthijs, Comarniceanu Antoaneta, Efdé Monique, Tengesdal Isak W, Schraa Kiki, Cleophas Maartje C P, Scribner Curtis L, Skouras Damaris B, Marchetti Carlo, Dinarello Charles A, Joosten Leo A B
Department of Internal Medicine, Radboud University Medical Center, Nijmegen, Netherlands (V Klück MD, K Schraa BSc, M C P Cleophas PhD, Prof C A Dinarello MD, Prof L A B Joosten PhD); Department of Rheumatology, VieCuri Medical Center, Venlo, Netherlands (T L Th A Jansen PhD, M Janssen PhD, A Comarniceanu MD, M Efdé MD); Olatec Therapeutics, New York, NY, USA (C L Scribner MD, D B Skouras MBA); Department of Medicine, University of Colorado, Aurora, CO, USA (I W Tengesdal MSc, C Marchetti PhD, Prof C A Dinarello); and Department of Medical Genetics, Iuliu Haţieganu University of Medicine and Pharmacy, Cluj-Napoca, Romania (Prof L A B Joosten).
Lancet Rheumatol. 2020 May;2(5):e270-e280. doi: 10.1016/s2665-9913(20)30065-5. Epub 2020 Apr 8.
Gout flares are driven by interleukin (IL)-1β. Dapansutrile inhibits the NLRP3 inflammasome and subsequent activation of IL-1β. In this study we aimed to investigate the safety and efficacy of orally administered dapansutrile in patients with a gout flare.
In this open-label, proof-of-concept, phase 2a trial, adult patients (aged 18-80 years) with a monoarticular monosodium urate crystal-proven gout flare were enrolled at an outpatient clinic in the Netherlands and sequentially assigned using a dose-adaptive design to receive 100 mg/day, 300 mg/day, 1000 mg/day, or 2000 mg/day oral dapansutrile for 8 days. The coprimary outcomes were change in patient-reported target joint pain from baseline to day 3 and from baseline to day 7, assessed in the per-protocol population (all patients who received at least 80% of the study drug and had no major protocol deviations). Safety was assessed in the intention-to-treat population. This trial is registered with the EU Clinical Trials Register, EudraCT 2016-000943-14, and is completed.
Between May 18, 2017, and Jan 21, 2019, 144 patients were assessed for eligibility, of whom 34 were enrolled and 29 were included in the per-protocol population (three patients were excluded due to receiving <80% of study drug and two had major protocol deviations): eight patients received 100 mg/day, seven received 300 mg/day, six received 1000 mg/day, and eight received 2000 mg/day. Between baseline and day 3, there was a mean reduction in patient-reported target joint pain of 52·4% (SD 32·94; p=0∙016) for the 100 mg/day group, 68·4% (34·29; p=0∙016) for the 300 mg/day group, 55·8% (44·90; p=0∙063) for the 1000 mg/day group, and 57·6% (38·72; p=0∙016) for the 2000 mg/day group. At day 7, there was a mean reduction of 82·1% (22·68; p=0∙031) for the 100 mg/day group, 84·2% (16·33; p=0∙016) for the 300 mg/day group, 68·9% (34·89; p=0∙031) for the 1000 mg/day group, and 83·9% (15·44; p=0∙008) for the 2000 mg/day group, compared to baseline. 25 (73·5%) of 34 patients reported a total of 45 treatment-emergent adverse events, most of which were metabolism and nutrition disorders (17 [37·8%]) and gastrointestinal disorders (ten [22·2%]). Two serious adverse events occurred during the study, admission to hospital because of worsening of gout flare at day 3, and admission to hospital because of coronary stenosis 18 days after the patient received their last dose; these were considered moderate in severity and unrelated to the study drug.
Dapansutrile is a specific NLRP3 inflammasome inhibitor with a satisfactory safety profile and efficacy in the reduction of target joint pain in this study. Future studies are needed to confirm the clinical potential of dapansutrile.
痛风发作由白细胞介素(IL)-1β驱动。达帕舒特rile抑制NLRP3炎性小体及随后的IL-1β激活。在本研究中,我们旨在调查口服达帕舒特rile治疗痛风发作患者的安全性和有效性。
在这项开放标签、概念验证的2a期试验中,荷兰一家门诊诊所招募了经单钠尿酸盐晶体证实为单关节痛风发作的成年患者(年龄18 - 80岁),并采用剂量适应性设计将其依次分配接受100毫克/天、300毫克/天、1000毫克/天或2000毫克/天的口服达帕舒特rile,持续8天。共同主要结局是在符合方案人群(所有接受至少80%研究药物且无重大方案偏离的患者)中评估从基线到第3天以及从基线到第7天患者报告的目标关节疼痛变化。在意向性治疗人群中评估安全性。该试验已在欧盟临床试验注册中心注册,EudraCT 2016 - 000943 - 14,且已完成。
在2017年5月18日至2019年1月21日期间,对144名患者进行了资格评估,其中34名患者入组,29名患者纳入符合方案人群(3名患者因接受研究药物不足80%被排除,2名患者有重大方案偏离):8名患者接受100毫克/天,7名患者接受300毫克/天,6名患者接受1000毫克/天,8名患者接受2000毫克/天。与基线相比,在第3天,100毫克/天组患者报告的目标关节疼痛平均减轻52.4%(标准差32.94;p = 0.016),300毫克/天组为68.4%(34.29;p = 0.016),1000毫克/天组为55.8%(44.90;p = 0.063),2000毫克/天组为57.6%(38.72;p = 0.016)。在第7天,100毫克/天组平均减轻82.1%(22.68;p = 0.031),300毫克/天组为84.2%(16.33;p = 0.016),1000毫克/天组为68.9%(34.89;p = 0.031),2000毫克/天组为83.9%(15.44;p = 0.008)。34名患者中有25名(73.5%)共报告了45起治疗中出现的不良事件,其中大多数是代谢和营养紊乱(17起[37.8%])以及胃肠道紊乱(10起[22.2%])。研究期间发生了两起严重不良事件,一起是在第3天因痛风发作恶化住院,另一起是患者最后一剂用药18天后因冠状动脉狭窄住院;这些不良事件被认为严重程度为中度且与研究药物无关。
达帕舒特rile是一种特异性NLRP3炎性小体抑制剂,在本研究中具有令人满意的安全性特征且在减轻目标关节疼痛方面有效。需要进一步研究以确认达帕舒特rile的临床潜力。
