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首页> 外文期刊>CPT: Pharmacometrics & Systems Pharmacology >A Quantitative Systems Pharmacology Model of Gaucher Disease Type 1 Provides Mechanistic Insight Into the Response to Substrate Reduction Therapy With Eliglustat
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A Quantitative Systems Pharmacology Model of Gaucher Disease Type 1 Provides Mechanistic Insight Into the Response to Substrate Reduction Therapy With Eliglustat

机译:Gaucher病型的定量系统药理模型提供了对eliglustat对基质还原疗法的反应提供机械洞察力

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摘要

Gaucher’s disease type 1 (GD1) leads to significant morbidity and mortality through clinical manifestations, such as splenomegaly, hematological complications, and bone disease. Two types of therapies are currently approved for GD1: enzyme replacement therapy (ERT), and substrate reduction therapy (SRT). In this study, we have developed a quantitative systems pharmacology (QSP) model, which recapitulates the effects of eliglustat, the only first‐line SRT approved for GD1, on treatment‐na?ve or patients with ERT‐stabilized adult GD1. This multiscale model represents the mechanism of action of eliglustat that leads toward reduction of spleen volume. Model capabilities were illustrated through the application of the model to predict ERT and eliglustat responses in virtual populations of adult patients with GD1, representing patients across a spectrum of disease severity as defined by genotype‐phenotype relationships. In summary, the QSP model provides a mechanistic computational platform for predicting treatment response via different modalities within the heterogeneous GD1 patient population.
机译:Gaucher的疾病1(GD1)通过临床表现导致显着的发病率和死亡率,例如脾肿大,血液学并发症和骨病。目前批准了两种类型的疗法:酶替代疗法(ERT)和底物还原治疗(SRT)。在这项研究中,我们开发了一种定量系统药理学(QSP)模型,其概述了Eliglustat的效果,批准了GD1的唯一一线SRT,在治疗 - Na'VE或患有ERT稳定的成年GD1的患者上。该多尺度模型代表了Eliglustat的作用机制,导致脾脏量减少。模型能力通过应用模型来预测成年患者的虚拟人群的ERT和Eliglustat反应,代表患者跨基因型 - 表型关系定义的疾病严重程度。总之,QSP模型提供了一种机械计算平台,用于通过异质GD1患者群体内的不同模式预测治疗响应。
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