| Literature DB >> 32744807 |
Anna Herland1,2,3, Ben M Maoz1,4,5,6, Edward A FitzGerald1, Thomas Grevesse1,4, Charles Vidoudez7, Sean P Sheehy1,4, Nikita Budnik4, Stephanie Dauth1,4, Robert Mannix1, Bogdan Budnik8, Kevin Kit Parker1,4, Donald E Ingber1,9,10.
Abstract
The functional state of the neurovascular unit (NVU), composed of the blood-brain barrier and the perivasculature that forms a dynamic interface between the blood and the central nervous system (CNS), plays a central role in the control of brain homeostasis and is strongly affected by CNS drugs. Human primary brain microvascular endothelium, astrocyte, pericyte, and neural cell cultures are often used to study NVU barrier functions as well as drug transport and efficacy; however, the proteomic and metabolomic responses of these different cell types are not well characterized. Culturing each cell type separately, using deep coverage proteomic analysis and characterization of the secreted metabolome, as well as measurements of mitochondrial activity, the responses of these cells under baseline conditions and when exposed to the NVU-impairing stimulant methamphetamine (Meth) are analyzed. These studies define the previously unknown metabolic and proteomic profiles of human brain pericytes and lead to improved characterization of the phenotype of each of the NVU cell types as well as cell-specific metabolic and proteomic responses to Meth.Entities:
Keywords: brain in vitro models; methamphetamine; neurovascular unit; primary cells
Year: 2020 PMID: 32744807 DOI: 10.1002/adbi.201900230
Source DB: PubMed Journal: Adv Biosyst ISSN: 2366-7478