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A Dynamic Quantitative Systems Pharmacology Model of Inflammatory Bowel Disease: Part 2 – Application to Current Therapies in Crohn’s Disease

机译:一种动态定量系统炎症肠病的药理学模型:第2部分 - 在克罗恩病疗法中的应用

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摘要

Inflammatory bowel disease (IBD) is a heterogeneic disease with a variety of treatments targeting different mechanisms. A multistate, mechanistic, mathematical model of IBD was developed in part 1 of this two‐part article series. In this paper, application of the model to predict response of key clinical biomarkers following different treatment options for Crohn’s disease was explored. Five therapies, representing four different mechanisms of action, were simulated in the model and longitudinal profiles of key clinical markers, C‐reactive protein and fecal calprotectin were compared with clinical observations. Model simulations provided an accurate match with both central tendency and variability observed in biomarker profiles. We also applied the model to predict biomarker and clinical response in an experimental, combination therapy of existing therapeutic options and provide possible mechanistic basis for the increased response. Overall, we present a validated, modular, mechanistic model construct, which can be applied to explore key biomarkers and clinical outcomes in IBD.
机译:炎症性肠病(IBD)是一种异质疾病,具有各种靶向不同机制的治疗方法。这款两部分文章系列的第1部分开发了IBD的多态,机械,数学模型。在本文中,探讨了模型的应用,以预测克罗恩疾病不同治疗选择后关键临床生物标志物的反应。将五种疗法,代表四种不同的作用机制,在关键临床标志物的模型和纵向谱中模拟,与临床观察相比,C-反应蛋白和粪便酸蛋白。模型仿真提供了一种准确的匹配,在生物标志物轮廓中观察到中央趋势和可变性。我们还将模型应用于预测现有治疗选择的实验组合治疗的生物标志物和临床反应,并为增加的反应提供可能的机制基础。总体而言,我们介绍了一种经过验证的模块化机械模型构建体,可应用于探索IBD中的关键生物标志物和临床结果。

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