The relationship among vedolizumab drug concentrations, biomarkers of inflammation, and clinical outcomes in a Canadian real-world study

C. H. Seow, J. K. Marshall, Stewart Erin, Christopher Pettengell, Ryan Ward, W. Afif
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Abstract

Therapeutic drug monitoring is used to optimize anti-tumour necrosis factor biologic effectiveness in inflammatory bowel disease, but its role with other biological classes is unclear. This study explores relationships between post-induction vedolizumab trough concentrations and biochemical outcomes in a real-world study of individuals with inflammatory bowel disease. This retrospective analysis of data from a national patient support program between 2018 and 2020, included 436 individuals with Crohn’s disease or ulcerative colitis receiving vedolizumab. Optimal vedolizumab concentration thresholds (at weeks 6 and 14) were determined based on their ability to predict biochemical normalization (week 30 faecal calprotectin [<250 µg/g], C-reactive protein [<5 mg/l]). Thresholds best associated with each outcome were evaluated in multivariate analyses. Among patients with Crohn’s disease, week 6 serum vedolizumab concentrations (>41.65 µg/ml) predicted normalization defined by C-reactive protein: Spearman correlation coefficient [ρ] = −0.26, P = 0.002 and multivariate analysis (MVA)—OR: 3.22, 95% CI: 1.32–7.87, P = 0.01, and at week 14 (>22.25 µg/ml): ρ = −0.38, P < 0.0001, and MVA—OR: 3.21, 95% CI: 1.26–8.17 but not faecal calprotectin. Similarly, among patients with ulcerative colitis, week 6 vedolizumab concentrations (>39.65 g/ml) predicted normalization defined by C-reactive protein: ρ = −0.26, P = 0.005 and MVA—OR: 4.03, 95% CI: 1.30–12.52, P = 0.016, and at week 14 (>17.35 µg/ml): ρ = −0.39, P = 0.0001 and MVA—OR: 6.95, 95% CI: 1.81–26.77, P = 0.005, but not faecal calprotectin. Induction and post-induction serum vedolizumab were not consistently associated with biochemical normalization. As such, proactive therapeutic drug monitoring for vedolizumab should not be routinely incorporated in a treat to target strategy for inflammatory bowel disease. NCT04567628.
加拿大一项真实世界研究中的维多珠单抗药物浓度、炎症生物标志物和临床结果之间的关系
治疗药物监测用于优化抗肿瘤坏死因子生物制剂在炎症性肠病中的疗效,但其在其他生物制剂中的作用尚不明确。本研究在一项针对炎症性肠病患者的真实世界研究中,探讨了诱导后韦多珠单抗谷浓度与生化结果之间的关系。 该研究对2018年至2020年间一项全国性患者支持计划的数据进行了回顾性分析,纳入了436名接受维多珠单抗治疗的克罗恩病或溃疡性结肠炎患者。最佳维多珠单抗浓度阈值(第6周和第14周)是根据其预测生化指标正常化的能力确定的(第30周粪便钙蛋白[41.65 µg/ml]预测了C反应蛋白定义的正常化:斯皮尔曼相关系数[ρ] = -0.26,P = 0.002,多变量分析(MVA)-OR:3.22,95% CI:1.32-7.87,P = 0.01;第 14 周(>22.25 µg/ml):ρ = -0.38,P <0.0001,MVA-OR:3.21,95% CI:1.26-8.17,但不能预测粪便钙蛋白。同样,在溃疡性结肠炎患者中,第 6 周维多利珠单抗浓度(>39.65 g/ml)可预测由 C 反应蛋白定义的正常化:ρ = -0.26,P = 0.005,MVA-OR:4.03,95% CI:1.30-12.52,P = 0.016;第 14 周(>17.35 µg/ml):ρ = -0.39,P = 0.0001,MVA-OR:6.95,95% CI:1.81-26.77,P = 0.005,但不能预测粪便钙蛋白。 诱导和诱导后血清维多珠单抗与生化指标正常化的关系并不一致。因此,在炎症性肠病的靶向治疗策略中,不应常规纳入对维多珠单抗的主动治疗药物监测。 NCT04567628。
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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