Journal
JOURNAL OF NEUROCHEMISTRY
Volume 118, Issue 5, Pages 826-840Publisher
WILEY-BLACKWELL
DOI: 10.1111/j.1471-4159.2011.07210.x
Keywords
Alzheimer's disease; amyloid beta-peptide; connexin; cytokines; diabetes mellitus; gap junctions; pannexin; stroke
Categories
Funding
- CRPCEN
- INSERM (France)
- CONICYT [24080055]
- FONDECYT [1070591]
- FONDEF [DO7I1086]
- ANILLO [ACT-71]
- NIH [NS55363, AR46798]
- INSERM (France
- Departement des Relations Internationales)
- Welch Foundation [Q-1507]
- Heart & Stroke Foundation of BC Yukon
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Inflammation contributes to neurodegeneration in post-ischemic brain, diabetes, and Alzheimer's disease. Participants in this inflammatory response include activation of microglia and astrocytes. We studied the role of microglia treated with amyloid-beta peptide (A beta) on hemichannel activity of astrocytes subjected to hypoxia in high glucose. Reoxygenation after 3 h hypoxia in high glucose induced transient astroglial permeabilization via Cx43 hemichannels and reduction in intercellular communication via Cx43 cell-cell channels. Both responses were greater and longer lasting in astrocytes previously exposed for 24 h to conditioned medium from A beta-treated microglia (CM-A beta). The effects of CM-A beta were mimicked by TNF-alpha and IL-1 beta and were abrogated by neutralizing TNF-alpha with soluble receptor and IL-1 beta with a receptor antagonist. Astrocytes under basal conditions protected neurons against hypoxia, but exposure to CM-A beta made them toxic to neurons subjected to a sub-lethal hypoxia/reoxygenation episode, revealing the additive nature of the insults. Astrocytes exposed to CM-A beta induced permeabilization of cortical neurons through activation of neuronal pannexin 1 (Panx1) hemichannels by ATP and glutamate released through astroglial Cx43 hemichannels. In agreement, inhibition of NMDA or P2X receptors only partially reduced the activation of neuronal Panx1 hemichannels and neuronal mortality, but simultaneous inhibition of both receptors completely prevented the neurotoxic response. Therefore, we suggest that responses to ATP and glutamate converge in activation of neuronal Panx1 hemichannels. Thus, we propose that blocking hemichannels expressed by astrocytes and/or neurons in the inflamed nervous system could represent a novel and alternative strategy to reduce neuronal loss in various pathological states including Alzheimer's disease, diabetes and ischemia.
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