Department of Gastroenterology and Hepatology, University Hospital Heidelberg, Heidelberg 69120, Germany,
Department of Medical Biometry, University Hospital Heidelberg, Heidelberg 69120, Germany.
World J Gastroenterol. 2019 Aug 21;25(31):4481-4492. doi: 10.3748/wjg.v25.i31.4481.
Ustekinumab was approved in Europe for the treatment of adults with moderate to severe Crohn's disease (CD) in 2016, and there is an urgent need for data on its everyday use.
To obtain data on the daily use of ustekinumab.
This is a retrospective monocentric study. Patients with moderate to severe CD who began ustekinumab therapy at the inflammatory bowel diseases outpatient clinic of the Heidelberg University Hospital between December 2016 and March 2018 were selected based on electronic patient files. The primary study endpoint was combined steroid-free clinical remission or steroid-free clinical response at 24 ± 6 wk of ustekinumab therapy. Secondary study endpoints were: achievement of mucosal healing, sonographic and magnetic resonance imaging response, biochemical response, the need for intestinal surgery within 24 ± 6 wk after treatment initiation, the occurrence of adverse events, treatment discontinuation due to nonresponse or adverse events, improvement of extraintestinal manifestations, clinical response at 48 ± 6 wk of therapy, and association of response with nucleotid oligodimerisation domain 2 mutations.
Fifty-seven patients with CD (5.3% anti-tumour necrosis factor α naïve, 63.2% having undergone at least one intestinal surgery) were included in the study. Twenty patients (35.1%) achieved steroid-free clinical remission, 6 (10.5%) steroid-free clinical response and 31 (54.4%) were non-responders. Treatment discontinuation due to adverse events occurred in two patients (3.5%). Male sex, the presence of extraintestinal manifestations and the use of steroids at baseline were predictors of nonresponse to ustekinumab therapy.
In a "real-world" treatment-refractory cohort of patients with CD, ustekinumab appeared efficacious and safe.
乌司奴单抗于 2016 年在欧洲获批用于治疗中重度克罗恩病(CD)成人患者,目前迫切需要其日常使用数据。
获取乌司奴单抗日常使用数据。
这是一项回顾性单中心研究。根据电子病历,选择 2016 年 12 月至 2018 年 3 月期间在海德堡大学医院炎症性肠病门诊开始乌司奴单抗治疗的中重度 CD 患者。主要研究终点为乌司奴单抗治疗 24±6 周时联合无激素临床缓解或无激素临床应答。次要研究终点为:黏膜愈合、超声和磁共振成像应答、生化应答、治疗开始后 24±6 周内需要肠手术、不良事件发生、因无应答或不良事件而停止治疗、肠外表现改善、治疗 48±6 周时的临床应答以及应答与核苷酸寡聚化结构域 2 突变的相关性。
共纳入 57 例 CD 患者(5.3%为抗肿瘤坏死因子α初治患者,63.2%曾接受过至少一次肠手术)。20 例(35.1%)患者达到无激素临床缓解,6 例(10.5%)达到无激素临床应答,31 例(54.4%)为无应答者。因不良事件而停止治疗的患者有 2 例(3.5%)。男性、存在肠外表现和基线时使用激素是乌司奴单抗治疗无应答的预测因素。
在治疗抵抗的 CD 患者真实世界队列中,乌司奴单抗似乎有效且安全。