Aqp4 stop codon readthrough facilitates amyloid-β clearance from the brain

Alzheimer's disease is initiated by the toxic aggregation of amyloid-β. Immunotherapeutics aimed at reducing amyloid beta are in clinical trials but with very limited success to date. Identification of orthogonal approaches for clearing amyloid beta may complement these approaches for treating...

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Published in:Brain (London, England : 1878) England : 1878), 2022-09, Vol.145 (9), p.2982-2990
Main Authors: Sapkota, Darshan, Florian, Colin, Doherty, Brookelyn M, White, Kelli M, Reardon, Kate M, Ge, Xia, Garbow, Joel R, Yuede, Carla M, Cirrito, John R, Dougherty, Joseph D
Format: Article
Language:English
Subjects:
Alzheimer Disease - metabolism
Amyloid beta-Peptides - metabolism
Animals
Aquaporin 4 - genetics
Aquaporin 4 - metabolism
Brain - metabolism
Codon, Terminator
Mice
Neurodegenerative Diseases - metabolism
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cited_by cdi_FETCH-LOGICAL-c388t-3ff59fd86d3a9706e1552a518ec734dacc7b6bfe80f6dc13461776522a95af083
cites cdi_FETCH-LOGICAL-c388t-3ff59fd86d3a9706e1552a518ec734dacc7b6bfe80f6dc13461776522a95af083
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container_issue 9
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container_title Brain (London, England : 1878)
container_volume 145
creator Sapkota, Darshan
Florian, Colin
Doherty, Brookelyn M
White, Kelli M
Reardon, Kate M
Ge, Xia
Garbow, Joel R
Yuede, Carla M
Cirrito, John R
Dougherty, Joseph D
description Alzheimer's disease is initiated by the toxic aggregation of amyloid-β. Immunotherapeutics aimed at reducing amyloid beta are in clinical trials but with very limited success to date. Identification of orthogonal approaches for clearing amyloid beta may complement these approaches for treating Alzheimer's disease. In the brain, the astrocytic water channel Aquaporin 4 is involved in clearance of amyloid beta, and the fraction of Aquaporin 4 found perivascularly is decreased in Alzheimer's disease. Further, an unusual stop codon readthrough event generates a conserved C-terminally elongated variant of Aquaporin 4 (AQP4X), which is exclusively perivascular. However, it is unclear whether the AQP4X variant specifically mediates amyloid beta clearance. Here, using Aquaporin 4 readthrough-specific knockout mice that still express normal Aquaporin 4, we determine that this isoform indeed mediates amyloid beta clearance. Further, with high-throughput screening and counterscreening, we identify small molecule compounds that enhance readthrough of the Aquaporin 4 sequence and validate a subset on endogenous astrocyte Aquaporin 4. Finally, we demonstrate these compounds enhance brain amyloid-β clearance in vivo, which depends on AQP4X. This suggests derivatives of these compounds may provide a viable pharmaceutical approach to enhance clearance of amyloid beta and potentially other aggregating proteins in neurodegenerative disease.
doi_str_mv 10.1093/brain/awac199
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Immunotherapeutics aimed at reducing amyloid beta are in clinical trials but with very limited success to date. Identification of orthogonal approaches for clearing amyloid beta may complement these approaches for treating Alzheimer's disease. In the brain, the astrocytic water channel Aquaporin 4 is involved in clearance of amyloid beta, and the fraction of Aquaporin 4 found perivascularly is decreased in Alzheimer's disease. Further, an unusual stop codon readthrough event generates a conserved C-terminally elongated variant of Aquaporin 4 (AQP4X), which is exclusively perivascular. However, it is unclear whether the AQP4X variant specifically mediates amyloid beta clearance. Here, using Aquaporin 4 readthrough-specific knockout mice that still express normal Aquaporin 4, we determine that this isoform indeed mediates amyloid beta clearance. 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source Oxford Journals Online
subjects Alzheimer Disease - metabolism
Amyloid beta-Peptides - metabolism
Animals
Aquaporin 4 - genetics
Aquaporin 4 - metabolism
Brain - metabolism
Codon, Terminator
Mice
Neurodegenerative Diseases - metabolism
title Aqp4 stop codon readthrough facilitates amyloid-β clearance from the brain
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