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Fate-mapping and functional dissection reveal perilous influence of type I interferon signaling in mouse brain aging.

Ethan R RoySanming LiSepideh SaroukhaniYanyu WangWei Cao
Published in: Molecular neurodegeneration (2024)
Overall, our study demonstrates pervasive IFN-I activity during normal mouse brain aging and reveals a pathogenic, pro-degenerative role played by microglial IFN-I signaling in perpetuating neuroinflammation, neuronal dysfunction, and molecular aggregation. These findings extend the understanding of a principal axis of age-related inflammation in the brain, one likely shared with multiple neurological disorders, and provide a rationale to modulate aberrant immune activation to mitigate neurodegenerative process at all stages.
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