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Publication : Deletion of the type-1 interferon receptor in APPSWE/PS1ΔE9 mice preserves cognitive function and alters glial phenotype.

First Author  Minter MR Year  2016
Journal  Acta Neuropathol Commun Volume  4
Issue  1 Pages  72
PubMed ID  27400725 Mgi Jnum  J:348496
Mgi Id  MGI:6838047 Doi  10.1186/s40478-016-0341-4
Citation  Minter MR, et al. (2016) Deletion of the type-1 interferon receptor in APPSWE/PS1DeltaE9 mice preserves cognitive function and alters glial phenotype. Acta Neuropathol Commun 4(1):72
abstractText  A neuro-inflammatory response is evident in Alzheimer's disease (AD), yet the precise mechanisms by which neuro-inflammation influences the progression of Alzheimer's disease (AD) remain poorly understood. Type-1 interferons (IFNs) are master regulators of innate immunity and have been implicated in multiple CNS disorders, however their role in AD progression has not yet been fully investigated. Hence, we generated APPSWE/PS1DeltaE9 mice lacking the type-1 IFN alpha receptor-1 (IFNAR1, APPSWE/PS1DeltaE9 x IFNAR1(-/-)) aged to 9 months to investigate the role of type-1 IFN signaling in a well-validated model of AD. APPSWE/PS1DeltaE9 x IFNAR1(-/-) mice displayed a modest reduction in Abeta monomer levels, despite maintenance of plaque deposition. This finding correlated with partial rescue of spatial learning and memory impairments in the Morris water maze in comparison to APPSWE/PS1DeltaE9 mice. Q-PCR identified a reduced type-1 IFN response and modulated pro-inflammatory cytokine secretion in APPSWE/PS1DeltaE9 x IFNAR1(-/-) mice compared to APPSWE/PS1DeltaE9 mice. Interestingly, immunohistochemistry displayed enhanced astrocyte reactivity but attenuated microgliosis surrounding amyloid plaque deposits in APPSWE/PS1DeltaE9 x IFNAR1(-/-) mice in comparison to APPSWE/PS1DeltaE9 mice. These APPSWE/PS1DeltaE9 x IFNAR1(-/-) microglial populations demonstrated an anti-inflammatory phenotype that was confirmed in vitro by soluble Abeta1-42 treatment of IFNAR1(-/-) primary glial cultures. Our findings suggest that modulating neuro-inflammatory responses by suppressing type-1 IFN signaling may provide therapeutic benefit in AD.
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