Dermatology Department, Hospital Vital Alvarez-Buylla de Mieres, Asturias, Spain.
Anaxomics Biotech SL, Barcelona, Spain.
Front Immunol. 2023 Sep 20;14:1212981. doi: 10.3389/fimmu.2023.1212981. eCollection 2023.
Psoriasis is a chronic immune-mediated inflammatory systemic disease with skin manifestations characterized by erythematous, scaly, itchy and/or painful plaques resulting from hyperproliferation of keratinocytes. Certolizumab pegol [CZP], a PEGylated antigen binding fragment of a humanized monoclonal antibody against TNF-alpha, is approved for the treatment of moderate-to-severe plaque psoriasis. Patients with psoriasis present clinical and molecular variability, affecting response to treatment. Herein, we utilized an approach to model the effects of CZP in a virtual population (vPop) with moderate-to-severe psoriasis. Our proof-of-concept study aims to assess the performance of our model in generating a vPop and defining CZP response variability based on patient profiles.
We built a quantitative systems pharmacology (QSP) model of a clinical trial-like vPop with moderate-to-severe psoriasis treated with two dosing schemes of CZP (200 mg and 400 mg, both every two weeks for 16 weeks, starting with a loading dose of CZP 400 mg at weeks 0, 2, and 4). We applied different modelling approaches: (i) an algorithm to generate vPop according to reference population values and comorbidity frequencies in real-world populations; (ii) physiologically based pharmacokinetic (PBPK) models of CZP dosing schemes in each virtual patient; and (iii) systems biology-based models of the mechanism of action (MoA) of the drug.
The combination of our different modelling approaches yielded a vPop distribution and a PBPK model that aligned with existing literature. Our systems biology and QSP models reproduced known biological and clinical activity, presenting outcomes correlating with clinical efficacy measures. We identified distinct clusters of virtual patients based on their psoriasis-related protein predicted activity when treated with CZP, which could help unravel differences in drug efficacy in diverse subpopulations. Moreover, our models revealed clusters of MoA solutions irrespective of the dosing regimen employed.
Our study provided patient specific QSP models that reproduced clinical and molecular efficacy features, supporting the use of computational methods as modelling strategy to explore drug response variability. This might shed light on the differences in drug efficacy in diverse subpopulations, especially useful in complex diseases such as psoriasis, through the generation of mechanistically based hypotheses.
银屑病是一种慢性免疫介导的炎症性系统性疾病,其皮肤表现为角质细胞过度增殖导致的红斑、鳞屑、瘙痒和/或疼痛斑块。培塞利珠单抗[CZP]是一种针对 TNF-α的人源化单克隆抗体的 PEG 化抗原结合片段,已被批准用于治疗中重度斑块型银屑病。患有银屑病的患者表现出临床和分子的变异性,影响治疗反应。在此,我们利用一种方法在一个中重度银屑病的虚拟人群(vPop)中模拟 CZP 的作用。我们的概念验证研究旨在评估我们的模型在生成 vPop 以及根据患者特征定义 CZP 反应变异性方面的性能。
我们构建了一个定量系统药理学(QSP)模型,模拟了一项临床试验样的 vPop,其中中重度银屑病患者接受两种 CZP 给药方案(200mg 和 400mg,每两周一次,共 16 周,在第 0、2 和 4 周给予 CZP 负荷剂量 400mg)。我们应用了不同的建模方法:(i)根据真实世界人群的参考人群值和合并症频率生成 vPop 的算法;(ii)每个虚拟患者的 CZP 给药方案的生理相关药代动力学(PBPK)模型;(iii)药物作用机制(MoA)的系统生物学模型。
我们不同建模方法的结合产生了一个 vPop 分布和一个与现有文献一致的 PBPK 模型。我们的系统生物学和 QSP 模型再现了已知的生物学和临床活性,呈现的结果与临床疗效测量相关。我们根据 CZP 治疗时预测的银屑病相关蛋白活性,对虚拟患者进行了聚类,这有助于揭示不同亚群中药物疗效的差异。此外,我们的模型揭示了 MoA 解决方案的聚类,而不管所使用的给药方案如何。
我们的研究提供了特定于患者的 QSP 模型,再现了临床和分子疗效特征,支持将计算方法作为建模策略用于探索药物反应变异性。这可能有助于揭示不同亚群中药物疗效的差异,特别是在银屑病等复杂疾病中,通过产生基于机制的假设。
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