Bronswijk Michiel, Moens Annick, Lenfant Matthias, Tops Sophie, Compernolle Griet, Van Assche Gert, Vermeire Séverine, Gils Ann, Ferrante Marc
Department of Gastroenterology and Hepatology, University Hospitals Leuven, KU Leuven, Leuven, Belgium.
Translational Research in GastroIntestinal Disorders (TARGID), Department of Chronic Diseases, Aging, and Metabolism (CHROMETA), KU Leuven, Leuven, Belgium.
Inflamm Bowel Dis. 2020 Mar 4;26(4):628-634. doi: 10.1093/ibd/izz167.
The use of infliximab biosimilar CT-P13 has increased in patients with inflammatory bowel disease. Nevertheless, doubts about switching from infliximab originator to biosimilar still exist among patients and health care professionals.
Our tertiary referral center underwent a mandatory switch from infliximab originator to CT-P13 in 2017. We investigated pharmacokinetics, efficacy, and safety of this switch. The primary endpoint was infliximab discontinuation within 6 months of switching. Secondary endpoints included loss of clinical remission, need for treatment optimization, adverse events, evolution of patient-reported outcome, C-reactive protein, infliximab trough levels, and antidrug-antibodies.
A total of 361 patients (54.0% male, 70.0% Crohn's disease, 55.6% in clinical remission) were enrolled. Infliximab discontinuation within 6 months was observed in 4%. Loss of clinical remission, adverse events, and antidrug-antibodies were identified in only 2.0%, 2.2%, and 1.1% of patients, respectively. C-reactive protein concentrations and infliximab trough levels remained stable. Independent factors associated with remission at 6 months were lower PRO2 at switch (HR 6.024; 95% CI, 4.878-8.000; P < 0.0001) and higher hemoglobin levels (HR 1.383; 95% CI, 1.044-2.299; P = 0.018).
Switching from infliximab originator to CT-P13 was not associated with an increased risk of treatment discontinuation, loss of clinical remission, or adverse events. No significant changes in infliximab trough levels or immunogenicity could be identified.
英夫利昔单抗生物类似药CT-P13在炎症性肠病患者中的使用有所增加。然而,患者和医护人员对于从英夫利昔单抗原研药转换为生物类似药仍存在疑虑。
我们的三级转诊中心于2017年强制从英夫利昔单抗原研药转换为CT-P13。我们调查了这种转换的药代动力学、疗效和安全性。主要终点是转换后6个月内停用英夫利昔单抗。次要终点包括临床缓解的丧失、治疗优化的需求、不良事件、患者报告结局的演变、C反应蛋白、英夫利昔单抗谷浓度和抗药抗体。
共纳入361例患者(男性占54.0%,克罗恩病占70.0%,临床缓解者占55.6%)。6个月内停用英夫利昔单抗的比例为4%。临床缓解丧失、不良事件和抗药抗体分别仅在2.0%、2.2%和1.1%的患者中出现。C反应蛋白浓度和英夫利昔单抗谷浓度保持稳定。与6个月时缓解相关的独立因素是转换时较低的PRO2(风险比6.024;95%置信区间,4.878 - 8.000;P < 0.0001)和较高的血红蛋白水平(风险比1.383;95%置信区间,1.044 - 2.299;P = 0.018)。
从英夫利昔单抗原研药转换为CT-P13与治疗中断风险增加、临床缓解丧失或不良事件无关。未发现英夫利昔单抗谷浓度或免疫原性有显著变化。
