Gastroenterology and Endoscopy, IRCCS San Raffaele Hospital and Vita-Salute San Raffaele University, Milan, Italy.
Inflammatory Bowel Disease Unit, Division of Gastroenterology and Hepatology, University of Calgary, Calgary, AB, Canada.
Lancet Gastroenterol Hepatol. 2024 Feb;9(2):133-146. doi: 10.1016/S2468-1253(23)00318-7. Epub 2023 Dec 14.
Many patients with moderately to severely active Crohn's disease do not respond to available therapies or lose response over time. The GALAXI-1 study previously found that three intravenous guselkumab dosages showed superior clinical and endoscopic outcomes over placebo at week 12 in patients with moderately to severely active Crohn's disease. We report the safety and efficacy of subcutaneous guselkumab maintenance regimens to week 48 in the GALAXI-1 study.
We did a phase 2, randomised, multicentre, double-blind trial. Adult patients with moderately to severely active Crohn's disease were randomly allocated with a computer-generated randomisation schedule to receive one of five treatment groups, with regimens consisting of an intravenous induction phase transitioning to a subcutaneous maintenance phase starting at week 12 in a treat-through design: (1) guselkumab 200→100 mg group (200 mg intravenous at weeks 0, 4, and 8, then 100 mg subcutaneous every 8 weeks; (2) guselkumab 600→200 mg group (600 mg intravenous at weeks 0, 4, and 8, then 200 mg subcutaneous every 4 weeks); (3) guselkumab 1200→200 mg group (1200 mg intravenous at weeks 0, 4, and 8, then 200 mg subcutaneous every 4 weeks); (4) ustekinumab group (approximately 6 mg/kg intravenous at week 0, then 90 mg subcutaneous every 8 weeks); or (5) placebo group (placebo induction followed by either placebo maintenance [for those with CDAI clinical response at week 12] or crossover to ustekinumab [for those without CDAI clinical response at week 12]). Endpoints assessed at week 48 included CDAI remission (CDAI score <150), endoscopic response (≥50% improvement from baseline in SES-CD or SES-CD score ≤2), and endoscopic remission (SES-CD score ≤2) in the primary efficacy analysis population of all randomised patients who received at least one dose of study drug, excluding those discontinued during a temporary study pause. Safety analyses included all randomised patients who received at least one study drug dose. This trial is registered at Clinical Trials.gov (NCT03466411) and is active but not recruiting.
Among 700 patients screened, 309 (112 biologic-naive; 197 biologic-experienced) were included in the primary efficacy analysis population: 61 in the guselkumab 200→100 mg group, 63 in the guselkumab 600→200 mg group, 61 in the guselkumab 1200→200 mg group, 63 in the ustekinumab group, and 61 in the placebo group. 126 (41%) women and 183 (59%) men were included, with median age 36·0 years (IQR 28·0-49·0). At week 48, the numbers of patients with CDAI clinical remission were 39 (64%) in the guselkumab 200→100 mg group, 46 (73%) in the guselkumab 600→200 mg group, 35 (57%) in the guselkumab 1200→200 mg group, and 37 (59%) in the ustekinumab group. The corresponding numbers of patients with endoscopic response were 27 (44%), 29 (46%), 27 (44%), and 19 (30%), respectively, and endoscopic remission was seen in 11 (18%), 11 (17%), 20 (33%), and four (6%) patients, respectively. In the placebo group, 15 patients were in CDAI clinical response at week 12 and continued placebo; of these, nine (60%) were in clinical remission at week 48. 44 patients in the placebo group were not in CDAI clinical response at week 12 and crossed over to ustekinumab; of these, 26 (59%) were in clinical remission at week 48. Up to week 48, adverse events frequencies in the safety population (n=360) were 46 (66%) of 70 patients (464·9 events per 100 patient-years of follow-up) in the placebo group, 163 (74%) of 220 patients (353·1 per 100 patient-years) in the three guselkumab groups combined, and 60 (85%) of 71 patients (350·7 per 100 patient-years) in the ustekinumab group. Among patients treated with guselkumab or ustekinumab, the most frequently reported infections up to week 48 were nasopharyngitis (25 [11%] of 220 guselkumab recipients, 12 [11%] of 114 ustekinumab recipients) and upper respiratory infections (13 [6%] guselkumab recipients, eight [7%] ustekinumab recipients). After week 12, one patient who responded to placebo induction and two guselkumab-treated patients had serious infections. No active tuberculosis, opportunistic infections, or deaths occurred.
Patients receiving guselkumab intravenous induction and subcutaneous maintenance treatment achieved high rates of clinical and endoscopic efficacy up to week 48. No new safety concerns were identified.
Janssen Research & Development.
许多中重度克罗恩病患者对现有疗法无反应或随着时间的推移失去反应。GALAXI-1 研究先前发现,三种静脉注射 Guselkumab 剂量在中重度克罗恩病患者中,在第 12 周时比安慰剂显示出更好的临床和内镜结局。我们报告了 GALAXI-1 研究中皮下 Guselkumab 维持方案至第 48 周的安全性和有效性。
我们进行了一项 2 期、随机、多中心、双盲试验。中重度克罗恩病成年患者通过计算机生成的随机分组方案,随机分配到五个治疗组中的一个,方案由静脉诱导期和皮下维持期组成,起始于第 12 周的治疗期:(1) Guselkumab 200→100mg 组(第 0、4 和 8 周静脉注射 200mg,然后每 8 周皮下注射 100mg);(2) Guselkumab 600→200mg 组(第 0、4 和 8 周静脉注射 600mg,然后每 4 周皮下注射 200mg);(3) Guselkumab 1200→200mg 组(第 0、4 和 8 周静脉注射 1200mg,然后每 4 周皮下注射 200mg);(4) Ustekinumab 组(第 0 周静脉注射约 6mg/kg,然后每 8 周皮下注射 90mg);或(5)安慰剂组(安慰剂诱导,然后根据第 12 周 CDAI 临床反应分为安慰剂维持组[CDAI 评分<150]或交叉至 Ustekinumab 组[第 12 周 CDAI 临床无反应])。第 48 周的主要疗效分析人群包括所有接受至少一剂研究药物的随机患者(在研究暂停期间停药的患者除外),评估的终点包括 CDAI 缓解(CDAI 评分<150)、内镜缓解(SES-CD 或 SES-CD 评分≥50%改善,且评分≤2)和内镜缓解(SES-CD 评分≤2)。安全性分析包括所有接受至少一剂研究药物的随机患者。这项试验在 ClinicalTrials.gov(NCT03466411)注册,目前处于活跃但不招募状态。
在 700 名筛查患者中,309 名(112 名生物初治;197 名生物经验)纳入主要疗效分析人群:61 名在 Guselkumab 200→100mg 组,63 名在 Guselkumab 600→200mg 组,61 名在 Guselkumab 1200→200mg 组,63 名在 Ustekinumab 组,61 名在安慰剂组。126 名(41%)为女性,183 名(59%)为男性,中位年龄为 36.0 岁(IQR 28.0-49.0)。第 48 周时,Guselkumab 200→100mg 组、Guselkumab 600→200mg 组、Guselkumab 1200→200mg 组和 Ustekinumab 组的 CDAI 临床缓解患者人数分别为 39(64%)、46(73%)、35(57%)和 37(59%)。相应的内镜缓解患者人数分别为 27(44%)、29(46%)、27(44%)和 19(30%),内镜缓解患者人数分别为 11(18%)、11(17%)、20(33%)和 4(6%)。安慰剂组中,15 名患者在第 12 周时 CDAI 临床反应继续接受安慰剂治疗;其中 9 名(60%)在第 48 周时临床缓解。安慰剂组中,44 名患者在第 12 周时 CDAI 临床无反应,交叉至 Ustekinumab 组;其中 26 名(59%)在第 48 周时临床缓解。截至第 48 周,安全性人群(n=360)的不良事件频率为:安慰剂组 70 名患者(464.9 例/100 患者年)为 46(66%),3 个 Guselkumab 组联合治疗的 220 名患者(353.1 例/100 患者年)为 163(74%),71 名 Ustekinumab 组患者(350.7 例/100 患者年)为 60(85%)。接受 Guselkumab 或 Ustekinumab 治疗的患者中,截至第 48 周最常报告的感染为鼻咽炎(220 名 Guselkumab 患者中有 25 名[11%],114 名 Ustekinumab 患者中有 12 名[11%])和上呼吸道感染(220 名 Guselkumab 患者中有 13 名[6%],114 名 Ustekinumab 患者中有 8 名[7%])。第 12 周后,1 名对安慰剂诱导有反应的患者和 2 名接受 Guselkumab 治疗的患者发生了严重感染。未发生活动性结核病、机会性感染或死亡。
接受 Guselkumab 静脉诱导和皮下维持治疗的患者在第 48 周时达到了较高的临床和内镜疗效。未发现新的安全性问题。
杨森研究实验室。
