Impact of Precision-Guided Dosing on Clinical Decision-Making and Health Care Utilization in Inflammatory Bowel Disease: A Retrospective Pretest/Posttest Real-World Study.

IF 1.8 Q3 GASTROENTEROLOGY & HEPATOLOGY

Crohn's & Colitis 360 Pub Date : 2025-06-24 eCollection Date: 2025-07-01 DOI:10.1093/crocol/otaf044

Ronen Arai, Adria Condino, Bincy P Abraham, Stephen B Hanauer, Udayakumar Navaneethan, Donald Lum, Syed A Hassan, Timothy Ritter, Esther A Torres, David Ziring, Harry Bray, Thierry Dervieux, Patricia Aragon Han, Terrence A Barrett

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Abstract

Background: Precision-guided dosing (PGD) is a personalized tool that optimizes clinical decision-making in the treatment of inflammatory bowel disease (IBD) with infliximab (IFX) and its biosimilars. PGD employs nonlinear mixed-effect models using patient-specific pharmacokinetic parameters to predict infliximab trough concentrations without the need to wait until the actual trough measurement. This approach calculates patient-specific clearance (CL) and provides tailored IFX dosing and administration intervals aimed at achieving target trough levels. Implementing PGD can enhance treatment outcomes in IBD patients and may potentially reduce healthcare expenditures.

Methods: We conducted a multicenter, retrospective study as a follow up to our previous clinical experience program (CEP). We aimed to evaluate the impact of PGD on clinical decision-making, patient outcomes, healthcare utilization, and expenditures. Treatment decisions included: IFX dose intensification, reduction, discontinuation, or continuation. Disease activity and healthcare resource utilization and costs in the 12 months pre- and post-test were compared. Disease activity was measured using the physician global assessment (PGA) as follows: remission (0), mild (1), moderate (2), and severe (3). Costs were calculated based on modeling pre-established literature data.

Results: Analysis of data from 82 patients across 7 states and Puerto Rico showed that PGD-driven therapeutic decision making led to IFX treatment intensification (27%) or discontinuation (7%) in patients with low forecasted trough IFX concentrations, high clearance, and presence of antidrug antibody. Conversely, IFX dosage was reduced (18%) or unchanged (48%) for patients with high IFX concentrations and low clearance. There was a significant association between forecasted trough IFX levels and treatment modifications (P < .001). High clearance (> 0.294 L/day) was significantly associated with therapy intensification (OR 6.22, 95% CI: 2.19-19.8; P < .001). Following PGD, disease activity improved significantly (observed mean difference in physician global assessment: 0.378, P = 0.008) and healthcare resource utilization decreased. Across the entire patient population, hospitalizations decreased from 30 events pretest to 5 events posttest (P < .001), leading to overall cost saving.

Conclusions: HCPs used the PGD test to guide treatment decisions. PGD-driven optimization of IFX therapy led to improved patient outcomes, lower healthcare utilization, and cost savings.

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精确指导给药对炎症性肠病临床决策和医疗保健利用的影响：一项回顾性测试前/测试后的真实世界研究

背景：精确引导给药（PGD）是一种个性化的工具，可优化英夫利昔单抗（IFX）及其生物类似药治疗炎症性肠病（IBD）的临床决策。PGD采用非线性混合效应模型，使用患者特异性药代动力学参数来预测英夫利昔单抗谷浓度，而无需等到实际谷值测量。该方法计算患者特异性清除率（CL），并提供量身定制的IFX剂量和给药间隔，旨在达到目标谷水平。实施PGD可以提高IBD患者的治疗效果，并可能潜在地减少医疗保健支出。方法：我们进行了一项多中心回顾性研究，作为我们之前临床经验计划（CEP）的随访。我们的目的是评估PGD对临床决策、患者预后、医疗保健利用和支出的影响。治疗决定包括：IFX剂量增强、减少、停药或继续。比较测试前后12个月的疾病活动度和医疗资源利用及费用。使用医师整体评估（PGA）测量疾病活动性如下：缓解(0)，轻度(1)，中度(2)和重度(3)。成本是根据预先建立的文献数据建模计算的。结果：来自7个州和波多黎各的82例患者的数据分析显示，pgd驱动的治疗决策导致IFX治疗强化（27%）或停药（7%），这些患者的预测通过IFX浓度低，清除率高，存在抗药抗体。相反，对于高IFX浓度和低清除率的患者，IFX剂量减少（18%）或不变（48%）。预测的谷底IFX水平与治疗修改之间存在显著相关性（P 0.294 L/天），与治疗强化显著相关(OR 6.22, 95% CI: 2.19-19.8；P = 0.008)，医疗资源利用率下降。在整个患者群体中，住院事件从测试前的30个事件减少到测试后的5个事件(P结论：HCPs使用PGD测试来指导治疗决策。pgd驱动的IFX治疗优化改善了患者的治疗效果，降低了医疗保健利用率，并节省了成本。

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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