Real-World Data on Short-Term and Long-Term Treatment Results of Ustekinumab in Patients with Steroid-Resistant/Dependent Ulcerative Colitis

Q2 Medicine

Inflammatory Intestinal Diseases Pub Date : 2023-10-05 DOI:10.1159/000534457

Yoriaki Komeda, George Tribonias, Masashi Kono, Kohei Handa, Shunsuke Omoto, Mamoru Takenaka, Satoru Hagiwara, Naoko Tsuji, Naoshi Nishida, Hiroshi Kashida, Masatoshi Kudo

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Abstract

Introduction: Ustekinumab is an IgG1 kappa monoclonal antibody directed against the common p40 subunit of interleukin-12 and interleukin-23, which activate Th1- and Th17-mediated immune responses, respectively. It has proven efficacy for the treatment of moderate to severe ulcerative colitis (UC) in the UNIFI Phase III clinical trial; however, data on its efficacy in the real world is limited. In this study, we aimed to assess the real-world efficacy of ustekinumab. Methods: This observational study included 30 patients with UC who received ustekinumab from April 2020 to April 2022. We examined demographic information, disease type and activity (Mayo score, partial Mayo score [PMS]), use of biologics, concomitant use of predonisolone (PSL), 8-week ustekinumab clinical response rate, remission induction rate, 44- and 152-week remission maintenance rate, continuation rate, and 44-week steroid-free remission rate. The primary outcomes were the short- and long-term efficacy of ustekinumab. Results: Included patients (53% women; mean age: 41.2 years [16–80 years]) had an average disease duration of 86 weeks. Mayo’s score (median) was 7.4 and the PMS was 5.4. Two (7%), 24 (80%), and four (13%) patients had a Mayo endoscopic sub-score (MES) of MES1, MES2, and MES3, respectively. The median serum CRP was 1.0 mg/dL. Five patients had no history of biotherapy (naive), while 8 and 17 had a history of one and two or more biologic agents, respectively. Eight patients were PSL-resistant and 22 were PSL-dependent. The 8-week clinical response rate was 73%, and the clinical remission induction rate was 70%. The remission maintenance rates at 44 and 152 weeks were 67% and 63%, respectively. The ustekinumab retention rate was 67% (86-week mean follow-up period). Regarding biologic failure cases, the clinical response rate in the failure group with up to one biologic agent (including naive cases) was 84.6%, which was higher than the 58.0% rate in the failure group with two or more biologic agents (p=0.06). Steroid-free remission rates at 44 and 152 weeks were 63% each. In the logistic regression analysis parameters for discontinuation of ustekinumab, only PMS remained significant after multivariate analysis (p=0.018). Conclusion: Our study showed short-term and long-term ustekinumab effectiveness, especially with comparative low disease activity.

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Ustekinumab治疗类固醇抵抗/依赖性溃疡性结肠炎患者的短期和长期治疗结果的真实世界数据

Ustekinumab是一种IgG1 kappa单克隆抗体，靶向白介素-12和白介素-23的常见p40亚基，分别激活Th1-和th17介导的免疫反应。在UNIFI III期临床试验中，它已被证明对治疗中度至重度溃疡性结肠炎(UC)有效;然而，关于其在现实世界中的有效性的数据是有限的。在这项研究中，我们旨在评估ustekinumab的实际疗效。方法:这项观察性研究包括30例UC患者，他们在2020年4月至2022年4月期间接受了ustekinumab治疗。我们检查了人口统计学信息、疾病类型和活动性(Mayo评分、部分Mayo评分[PMS])、生物制剂的使用、同时使用泼尼松龙(PSL)、8周ustekinumab临床缓解率、缓解诱导率、44周和152周缓解维持率、延续率和44周无类固醇缓解率。主要结局是ustekinumab的短期和长期疗效。结果:纳入患者(女性53%;平均年龄41.2岁[16-80岁]，平均病程86周。Mayo评分(中位数)为7.4,PMS为5.4。2例(7%)、24例(80%)和4例(13%)患者的梅奥内镜亚评分(MES)分别为MES1、MES2和MES3。血清CRP中位数为1.0 mg/dL。5例患者没有生物治疗史(初治)，8例和17例分别有一种和两种或两种以上生物药物治疗史。8例psl耐药，22例psl依赖。8周临床缓解率为73%，临床缓解诱导率为70%。44周和152周的缓解维持率分别为67%和63%。ustekinumab保留率为67%(平均随访86周)。对于生物制剂治疗失败的病例，最多使用一种生物制剂(包括初治病例)治疗失败组的临床有效率为84.6%，高于使用两种或两种以上生物制剂治疗失败组的58.0% (p=0.06)。44周和152周无类固醇缓解率各为63%。在ustekinumab停药的logistic回归分析参数中，多因素分析后，只有PMS仍然显著(p=0.018)。结论:我们的研究显示了ustekinumab的短期和长期有效性，特别是在疾病活动性相对较低的情况下。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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