4.3 Article

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

Journal

CPT-PHARMACOMETRICS & SYSTEMS PHARMACOLOGY
Volume 4, Issue 10, Pages 585-594

Publisher

WILEY
DOI: 10.1002/psp4.12010

Keywords

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Funding

  1. DARPA Microphysiological Systems Program [W911NF-12-20039]
  2. NIH Microphysiological Systems Program [4-UH3-TR00049603]
  3. MIT Center for Environmental Health Sciences (NIEHS) [P30-ES002109]

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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.

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