Protection against hypoxia-induced increase in blood-brain barrier permeability: Role of tight junction proteins and NFκB
2003
Co-culture with glial cells and glia-conditioned media can induce
blood-brain barrier properties in microvessel endothelial cells and protect
against hypoxia-induced blood-brain barrier breakdown. We examined the effect
of two types of glia-conditioned media on brain microvessel endothelial cell
permeability and tight junction protein expression, and studied potential
mechanisms of action. We found that C6-glioma-conditioned media, but not rat
astrocyte-conditioned media, protected against an increase in permeability
induced by exposure to 1% oxygen for 24 hours. This hypoxic stress caused an
increase in the expression of tight junction proteins claudin-1 and actin,
particularly in cells treated with C6-conditioned media. We found that
C6-conditioned media has a significantly higher level of both basic fibroblast
growth factor and vascular endothelial growth factor. Treatment with
C6-conditioned media for 1 or 3 days protects against hypoxia-induced
permeability increases, and this protective effect may be mediated by signal
transduction pathways terminating at the transcription factor NFκB.
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