Adalimumab Biosimilars Demonstrate Long-Term Durability and Cost-Effectiveness in Paediatric Inflammatory Bowel Disease: A Real-World Two-Centre European Cohort Study.

IF 5.3 Q1 MEDICINE, RESEARCH & EXPERIMENTAL

Biologics : Targets & Therapy Pub Date : 2025-04-29 eCollection Date: 2025-01-01 DOI:10.2147/BTT.S511248

Silvana Ancona, Katherine Armstrong, Chiara Longo, Rosalind Rabone, Victoria Merrick, Paul Henderson, Paolo Gandullia, David C Wilson, Serena Arrigo, Richard K Russell

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引用次数: 0

Abstract

Purpose: Adalimumab biosimilars are increasingly used in paediatric Inflammatory Bowel Disease (PIBD), but data remain limited. This study assessed their durability, efficacy, safety and cost implications in PIBD.

Patients and methods: Consecutive PIBD patients who started adalimumab biosimilars between October 2018 and December 2023 at two centres in Scotland and Italy, with at least 6 months follow-up, were included. Demographic, disease, treatment, and adverse event data were collected. Disease activity was assessed at baseline, 6, 12, 24, 36 months, and at last follow-up. Durability was evaluated using Kaplan-Meier analysis.

Results: In total 130 patients (81 males; median age 12.3 years) were included (115 Crohn's Disease, 7 Ulcerative Colitis, 8 IBD unclassified). The biosimilars were ABP 501 (85%), GP2017 (14%), SB5 (1%); 41 (32%) patients switched from originator. After a median follow-up of 26 months, 87/130 (67%) patients remained on biosimilars, while 43 discontinued at a median of 14 months. Durability probabilities were 93%, 86%, 75%, 62%, and 57% at 6, 12, 24, 36, and 54 months, respectively. Patients previously exposed to ADA originator had a lower risk of biosimilar failure (hazard ratio, adjusted for age at diagnosis: 0.51 [95% confidence interval: 0.26-0.99], p=0.047). Trough levels ≥11.6 μg/mL at 6 months were associated with greater durability (AUC=0.68, p=0.007). Adverse events occurred in 46/130 patients, mainly psoriasis and injection site reactions (13% each), with one lymphoma. Estimated cost savings were 5,030€ per patient/year.

Conclusion: This real-life study demonstrated high durability and remission rates for adalimumab biosimilars in PIBD, confirming their clinical, cost-effectiveness and safety profile in children.

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阿达木单抗生物仿制药在儿童炎症性肠病中的长期耐久性和成本效益：一项真实世界的欧洲双中心队列研究

目的：阿达木单抗生物类似药越来越多地用于儿科炎症性肠病（PIBD），但数据仍然有限。本研究评估了它们在PIBD中的耐久性、有效性、安全性和成本影响。患者和方法：纳入2018年10月至2023年12月在苏格兰和意大利两个中心连续开始阿达木单抗生物仿制药的PIBD患者，随访至少6个月。收集人口统计、疾病、治疗和不良事件数据。在基线、6个月、12个月、24个月、36个月和最后随访时评估疾病活动性。使用Kaplan-Meier分析评估耐久性。结果：共130例患者(男性81例；中位年龄12.3岁)纳入（克罗恩病115例，溃疡性结肠炎7例，IBD未分类8例）。生物仿制药分别为ABP 501（85%）、GP2017（14%）、SB5 (1%)；41例（32%）患者从起始者切换。在中位随访26个月后，130例患者中有87例（67%）继续使用生物仿制药，43例在中位随访14个月后停药。在6、12、24、36和54个月时，耐久性概率分别为93%、86%、75%、62%和57%。先前暴露于ADA原药的患者生物仿制药失败的风险较低（根据诊断时年龄调整的风险比：0.51[95%置信区间：0.26-0.99],p=0.047）。6个月时波谷水平≥11.6 μg/mL与更长的持久性相关（AUC=0.68, p=0.007）。130例患者中有46例发生不良事件，主要为牛皮癣和注射部位反应（各占13%），1例淋巴瘤。估计每位患者每年可节省费用5030欧元。结论：这项现实生活中的研究表明，阿达木单抗生物类似药在PIBD中的耐久性和缓解率很高，证实了它们在儿童中的临床、成本效益和安全性。

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