| Literature DB >> 35311644 |
Felicia Reinitz1, Elizabeth Y Chen1, Benedetta Nicolis di Robilant1, Bayarsaikhan Chuluun2, Jane Antony1, Robert C Jones3, Neha Gubbi1, Karen Lee1, William Hai Dang Ho1, Sai Saroja Kolluru3, Dalong Qian1, Maddalena Adorno1, Katja Piltti4, Aileen Anderson4, Michelle Monje1, H Craig Heller2, Stephen R Quake3, Michael F Clarke1.
Abstract
Alzheimer's disease (AD) is a progressive neurodegenerative disease observed with aging that represents the most common form of dementia. To date, therapies targeting end-stage disease plaques, tangles, or inflammation have limited efficacy. Therefore, we set out to identify a potential earlier targetable phenotype. Utilizing a mouse model of AD and human fetal cells harboring mutant amyloid precursor protein, we show cell intrinsic neural precursor cell (NPC) dysfunction precedes widespread inflammation and amyloid plaque pathology, making it the earliest defect in the evolution of the disease. We demonstrate that reversing impaired NPC self-renewal via genetic reduction of USP16, a histone modifier and critical physiological antagonist of the Polycomb Repressor Complex 1, can prevent downstream cognitive defects and decrease astrogliosis in vivo. Reduction of USP16 led to decreased expression of senescence gene Cdkn2a and mitigated aberrant regulation of the Bone Morphogenetic Signaling (BMP) pathway, a previously unknown function of USP16. Thus, we reveal USP16 as a novel target in an AD model that can both ameliorate the NPC defect and rescue memory and learning through its regulation of both Cdkn2a and BMP signaling.Entities:
Keywords: Alzheimer's; mouse; neural stem cells; neurodegeneration; regenerative medicine; stem cells
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Year: 2022 PMID: 35311644 PMCID: PMC9122497 DOI: 10.7554/eLife.66037
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.713