Ferrante Marc, D'Haens Geert, Jairath Vipul, Danese Silvio, Chen Minhu, Ghosh Subrata, Hisamatsu Tadakazu, Kierkus Jaroslaw, Siegmund Britta, Bragg Sonja Michelle, Crandall Wallace, Durand Frederick, Hon Emily, Lin Zhantao, Lopes Michelle Ugolini, Morris Nathan, Protic Marijana, Carlier Hilde, Sands Bruce E
Department of Gastroenterology and Hepatology, University Hospitals Leuven, KU Leuven, Leuven, Belgium.
Inflammatory Bowel Disease Centre, Amsterdam University Medical Center, Amsterdam, Netherlands.
Lancet. 2024 Dec 14;404(10470):2423-2436. doi: 10.1016/S0140-6736(24)01762-8. Epub 2024 Nov 21.
Mirikizumab, a humanised monoclonal antibody that inhibits IL-23p19, is effective in moderate-to-severe ulcerative colitis. We aimed to evaluate the efficacy and safety of mirikizumab in patients with moderately-to-severely active Crohn's disease.
VIVID-1 was a global phase 3, randomised, double-blind, double-dummy, placebo-controlled and active-controlled, treat-through study. The study enrolled adult patients at 324 sites (hospitals or medical centres, clinical practices, and clinical research sites) in 33 countries across Europe, Asia, North America, Central America, South America, and Australia. Adult patients with moderately-to-severely active Crohn's disease and previous inadequate response, loss of response, or intolerance to one or more approved biological therapies or conventional therapies were randomly assigned 6:3:2 to receive mirikizumab 900 mg intravenously at weeks 0, 4, and 8, then 300 mg subcutaneously every 4 weeks from weeks 12 to 52; ustekinumab about 6 mg/kg intravenously at week 0, then 90 mg subcutaneously every 8 weeks from weeks 8 to 52; or placebo. The coprimary endpoints assessing superiority of mirikizumab over placebo were composite endpoints: patient-reported outcome (PRO) clinical response at week 12 and endoscopic response at week 52 (endoscopic response-composite), and PRO clinical response at week 12 and Crohn's Disease Activity Index (CDAI) clinical remission at week 52 (CDAI clinical remission-composite). The adjusted risk differences were calculated, and the comparison was performed by the Cochran-Mantel-Haenszel test. Non-responder imputation was used. VIVID-1 was registered on ClinicalTrials.gov, NCT03926130, and is now complete.
Between July 23, 2019, and Aug 23, 2023, 1150 patients were randomly assigned and received study treatment (safety population); 1065 patients were included in the efficacy population and received mirikizumab (n=579), ustekinumab (n=287), or placebo (n=199). Both coprimary endpoints were met: endoscopic response-composite was reached in 220 (38·0%) of 579 patients on mirikizumab versus 18 (9·0%) of 199 on placebo (99·5% CI 20·6-36·8; p<0·0001); CDAI clinical remission-composite was reached in 263 (45·4%) of 579 patients on mirikizumab versus 39 (19·6%) of 199 patients on placebo (99·5% CI 15·9-35·6; p<0·0001). The incidence rates of overall adverse events and discontinuations in patients treated with mirikizumab were lower compared with placebo. The most common adverse event across the three groups was COVID-19. Serious adverse events were reported in 65 (10·3%) of 630 patients on mirikizumab, 33 (10·7%) of 309 patients on ustekinumab, and 36 (17·1%) of 211 patients on placebo. There were three deaths during VIVID-1, one in the ustekinumab group, and two in the placebo group, including one in a placebo non-responder who switched to mirikizumab after week 12. None of the deaths were considered related to the study drug. The safety of mirikizumab in Crohn's disease was consistent with its known favourable profile.
Mirikizumab was safe and effective as induction and maintenance treatment for patients with moderately-to-severely active Crohn's disease who had intolerance, inadequate response, or loss of response to standard therapy.
Eli Lilly and Company.
Mirikizumab是一种抑制IL-23p19的人源化单克隆抗体,对中度至重度溃疡性结肠炎有效。我们旨在评估Mirikizumab在中度至重度活动性克罗恩病患者中的疗效和安全性。
VIVID-1是一项全球3期、随机、双盲、双模拟、安慰剂对照和活性对照的持续治疗研究。该研究在欧洲、亚洲、北美、中美洲、南美洲和澳大利亚的33个国家的324个地点(医院或医疗中心、临床诊所和临床研究地点)招募成年患者。患有中度至重度活动性克罗恩病且既往对一种或多种获批的生物疗法或传统疗法反应不足、反应丧失或不耐受的成年患者被随机分配,比例为6:3:2,分别接受在第0、4和8周静脉注射900mg Mirikizumab,然后从第12周开始至第52周每4周皮下注射300mg;在第0周静脉注射约6mg/kg优特克单抗,然后从第8周开始至第52周每8周皮下注射90mg;或安慰剂。评估Mirikizumab优于安慰剂的共同主要终点是复合终点:第12周的患者报告结局(PRO)临床反应和第52周的内镜反应(内镜反应复合终点),以及第12周的PRO临床反应和第52周的克罗恩病活动指数(CDAI)临床缓解(CDAI临床缓解复合终点)。计算调整后的风险差异,并通过 Cochr an-Mantel-Haenszel检验进行比较。采用无反应者插补法。VIVID-1已在ClinicalTrials.gov上注册,编号为NCT03926130,现已完成。
在2019年7月23日至2023年8月23日期间,1150名患者被随机分配并接受研究治疗(安全人群);1065名患者被纳入疗效人群并接受了Mirikizumab(n = 579)、优特克单抗(n = 287)或安慰剂(n = 199)治疗。两个共同主要终点均达到:接受Mirikizumab治疗的579名患者中有220名(38.0%)达到内镜反应复合终点,而接受安慰剂治疗的199名患者中有18名(9.0%)达到(99.5%CI 20.6 - 36.8;p < 0.0001);接受Mirikizumab治疗的579名患者中有263名(45.4%)达到CDAI临床缓解复合终点,而接受安慰剂治疗的199名患者中有39名(19.6%)达到(99.5%CI 15.9 - 35.6;p < 0.0001)。与安慰剂相比,接受Mirikizumab治疗的患者总体不良事件和停药发生率较低。三组中最常见的不良事件是COVID-19。接受Mirikizumab治疗的630名患者中有65名(10.3%)报告了严重不良事件,接受优特克单抗治疗的309名患者中有33名(10.7%),接受安慰剂治疗的211名患者中有36名(17.1%)。VIVID-1期间有3例死亡,优特克单抗组1例,安慰剂组2例,其中1例是在第12周后从安慰剂组转为接受Mirikizumab治疗的无反应者。所有死亡均被认为与研究药物无关。Mirikizumab在克罗恩病中的安全性与其已知的良好特征一致。
对于对标准治疗不耐受、反应不足或反应丧失的中度至重度活动性克罗恩病患者,Mirikizumab作为诱导和维持治疗是安全有效的。
礼来公司。
