Distinct trajectories of symptomatic response in ulcerative colitis during filgotinib therapy: A post hoc analysis from the SELECTION study.

IF 5.8 2区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
United European Gastroenterology Journal Pub Date : 2024-11-01 Epub Date: 2024-10-25 DOI:10.1002/ueg2.12686
Stefan Schreiber, Brian G Feagan, Edouard Louis, Tadakazu Hisamatsu, Toshifumi Hibi, Louis Dron, Corinne Jamoul, Haridarshan Patel, Kristina Harris, Virginia Taliadouros, Alessandra Oortwijn, Laurent Peyrin-Biroulet
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引用次数: 0

Abstract

Background: Filgotinib is an oral, once-daily, Janus kinase 1 preferential inhibitor approved for treatment of ulcerative colitis (UC) following the phase 2b/3 SELECTION trial. Identification of patient populations and factors associated with long-term treatment response trajectories may improve UC management.

Objective: We aimed to identify and describe distinct patient subgroups of response to filgotinib based on partial Mayo Clinic Score (pMCS) trajectories over time.

Methods: In these post hoc analyses of SELECTION, group-based trajectory modeling (GBTM) was applied to pMCS to describe groups of distinct, symptom-based patient trajectories using data from patients who responded to filgotinib 200 or 100 mg and continued receiving filgotinib up to week 58. Patient demographics, disease characteristics, and week 10 response were compared between the groups. Achievement of a patient-level multi-component endpoint of comprehensive disease control (CDC) was assessed in each group.

Results: GBTM identified five distinct patient populations with different response trajectories; 67.5% of patients had beneficial trajectories. The beneficial trajectory groups generally had higher proportions of patients who were recently diagnosed (<1 year), were receiving filgotinib 200 mg and were biologic-naive versus the relapsing trajectory groups (4%-9% vs. 4%-5%; 43%-65% vs. 36%-46%; 54%-70% vs. 35%-58%, respectively). Furthermore, 55.4% of patients had sustained beneficial trajectories, with low baseline endoscopic subscores (≥43% of patients had a subscore of 2) and strong week 10 FCP responses (≥61% of patients with >50% decrease in FCP from baseline). Sustained beneficial trajectory groups had a higher probability of achieving CDC at week 58 than other groups (31%-32% vs. 0%-7%).

Conclusions: Beneficial long-term response trajectories and achievement of CDC with filgotinib were associated with being biologic-naive and having less severe disease at baseline. Early estimation of sustained and CDC may facilitate patient identification and development of personalized management strategies in UC.

Clinicaltrials:

Gov identifier: NCT02914522.

菲戈替尼治疗期间溃疡性结肠炎症状反应的不同轨迹:SELECTION 研究的事后分析。
背景介绍Filgotinib 是一种口服、每日一次的 Janus 激酶 1 首选抑制剂,在 2b/3 期 SELECTION 试验后被批准用于治疗溃疡性结肠炎 (UC)。确定与长期治疗反应轨迹相关的患者人群和因素可改善 UC 的管理:我们旨在根据梅奥诊所部分评分(pMCS)随时间变化的轨迹,识别并描述对非格替尼反应的不同患者亚群:在SELECTION的这些事后分析中,基于组的轨迹建模(GBTM)被应用于pMCS,以描述基于症状的不同患者组的轨迹,这些数据来自对非格替尼200或100毫克有反应并继续接受非格替尼治疗至第58周的患者。对各组患者的人口统计学特征、疾病特征和第10周反应进行了比较。对每组患者实现患者层面的综合疾病控制(CDC)多组分终点进行了评估:GBTM确定了具有不同应答轨迹的五种不同患者群体;67.5%的患者具有获益轨迹。受益轨迹组中最近确诊的患者比例普遍较高(FCP较基线下降50%)。持续有益轨迹组在第58周达到CDC的概率高于其他组别(31%-32% vs. 0%-7%):结论:菲戈替尼的长期获益反应轨迹和达到CDC与基线时未使用生物制剂和病情较轻有关。对持续反应和CDC的早期评估有助于UC患者的识别和个性化管理策略的制定:Gov 标识符:NCT02914522。
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来源期刊
United European Gastroenterology Journal
United European Gastroenterology Journal GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
10.50
自引率
13.30%
发文量
147
期刊介绍: United European Gastroenterology Journal (UEG Journal) is the official Journal of the United European Gastroenterology (UEG), a professional non-profit organisation combining all the leading European societies concerned with digestive disease. UEG’s member societies represent over 22,000 specialists working across medicine, surgery, paediatrics, GI oncology and endoscopy, which makes UEG a unique platform for collaboration and the exchange of knowledge.
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