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Quantitative Systems Pharmacology Approaches Applied to Microphysiological Systems (MPS): Data Interpretation and Multi-MPS Integration

机译:应用于微生理系统(MPS)的定量系统药理学方法:数据解释和多MPS集成

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摘要

Our goal in developing Microphysiological Systems (MPS) technology is to provide an improved approach for more predictive preclinical drug discovery via a highly integrated experimental/computational paradigm. Success will require quantitative characterization of MPSs and mechanistic analysis of experimental findings sufficient to translate resulting insights from in vitro to in vivo. We describe herein a systems pharmacology approach to MPS development and utilization that incorporates more mechanistic detail than traditional pharmacokinetic/pharmacodynamic (PK/PD) models. A series of studies illustrates diverse facets of our approach. First, we demonstrate two case studies: a PK data analysis and an inflammation response––focused on a single MPS, the liver/immune MPS. Building on the single MPS modeling, a theoretical investigation of a four-MPS interactome then provides a quantitative way to consider several pharmacological concepts such as absorption, distribution, metabolism, and excretion in the design of multi-MPS interactome operation and experiments.
机译:我们开发微生理系统(MPS)技术的目标是通过高度集成的实验/计算范例,为更可预测的临床前药物发现提供一种改进的方法。成功将需要对MPS进行定量表征,并对实验结果进行机理分析,以将所得到的见解从体外转化为体内。我们在这里描述了MPS开发和利用的系统药理学方法,该方法结合了比传统药代动力学/药效学(PK / PD)模型更多的机械细节。一系列研究说明了我们方法的各个方面。首先,我们展示了两个案例研究:PK数据分析和炎症反应-集中于单个MPS,即肝脏/免疫MPS。在单个MPS建模的基础上,对四个MPS相互作用组进行理论研究,然后提供一种定量方法,以考虑在多个MPS相互作用组的操作和实验设计中考虑几种药理学概念,例如吸收,分布,代谢和排泄。

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