A linked organ-on-chip model of the human neurovascular unit reveals the metabolic coupling of endothelial and neuronal cells
Author(s) -
Ben M. Maoz,
Anna Herland,
Edward A. Fitzgerald,
Thomas Grevesse,
Charles Vidoudez,
Alan R. Pacheco,
Sean P. Sheehy,
TaeEun Park,
Stephanie Dauth,
Robert Mannix,
Nikita Budnik,
Kevin L. Shores,
Alexander Cho,
Janwroth,
Daniel Segrè,
Bogdan Budnik,
Donald E. Ingber,
Kevin Kit Parker
Publication year - 2018
Publication title -
nature biotechnology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 15.358
H-Index - 445
eISSN - 1546-1696
pISSN - 1087-0156
DOI - 10.1038/nbt.4226
Subject(s) - blood–brain barrier , neuroscience , compartment (ship) , central nervous system , efflux , homeostasis , mechanism (biology) , pharmacology , endothelium , methamphetamine , biology , chemistry , microbiology and biotechnology , biochemistry , oceanography , philosophy , epistemology , geology , endocrinology
The neurovascular unit (NVU) regulates metabolic homeostasis as well as drug pharmacokinetics and pharmacodynamics in the central nervous system. Metabolic fluxes and conversions over the NVU rely on interactions between brain microvascular endothelium, perivascular pericytes, astrocytes and neurons, making it difficult to identify the contributions of each cell type. Here we model the human NVU using microfluidic organ chips, allowing analysis of the roles of individual cell types in NVU functions. Three coupled chips model influx across the blood-brain barrier (BBB), the brain parenchymal compartment and efflux across the BBB. We used this linked system to mimic the effect of intravascular administration of the psychoactive drug methamphetamine and to identify previously unknown metabolic coupling between the BBB and neurons. Thus, the NVU system offers an in vitro approach for probing transport, efficacy, mechanism of action and toxicity of neuroactive drugs.
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