The APOE-R136S mutation protects against APOE4-driven Tau pathology, neurodegeneration and neuroinflammation

被引:0
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作者
Maxine R. Nelson
Peng Liu
Ayushi Agrawal
Oscar Yip
Jessica Blumenfeld
Michela Traglia
Min Joo Kim
Nicole Koutsodendris
Antara Rao
Brian Grone
Yanxia Hao
Seo Yeon Yoon
Qin Xu
Samuel De Leon
Tenzing Choenyi
Reuben Thomas
Francisco Lopera
Yakeel T. Quiroz
Joseph F. Arboleda-Velasquez
Eric M. Reiman
Robert W. Mahley
Yadong Huang
机构
[1] Gladstone Institutes,Gladstone Institute of Neurological Disease
[2] University of California,Biomedical Sciences Graduate Program
[3] San Francisco,Gladstone Institute of Data Science and Biotechnology
[4] Gladstone Institutes,Neuroscience Graduate Program
[5] University of California,Developmental and Stem Cell Biology Graduate Program
[6] San Francisco,Gladstone Center for Translational Advancement
[7] University of California,Departments of Neurology and Psychiatry
[8] San Francisco,Schepens Eye Research Institute of Mass Eye and Ear and Department of Ophthalmology
[9] Gladstone Institutes,Department of Pathology
[10] Grupo de Neurociencias de Antioquia de la Universidad de Antioquia,Department of Medicine
[11] Massachusetts General Hospital and Harvard Medical School,Department of Neurology
[12] Harvard Medical School,undefined
[13] Banner Alzheimer’s Institute,undefined
[14] University of Arizona,undefined
[15] University of California,undefined
[16] San Francisco,undefined
[17] University of California,undefined
[18] San Francisco,undefined
[19] University of California,undefined
[20] San Francisco,undefined
来源
Nature Neuroscience | 2023年 / 26卷
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摘要
Apolipoprotein E4 (APOE4) is the strongest genetic risk factor for late-onset Alzheimer’s disease (LOAD), leading to earlier age of clinical onset and exacerbating pathologies. There is a critical need to identify protective targets. Recently, a rare APOE variant, APOE3-R136S (Christchurch), was found to protect against early-onset AD in a PSEN1-E280A carrier. In this study, we sought to determine if the R136S mutation also protects against APOE4-driven effects in LOAD. We generated tauopathy mouse and human iPSC-derived neuron models carrying human APOE4 with the homozygous or heterozygous R136S mutation. We found that the homozygous R136S mutation rescued APOE4-driven Tau pathology, neurodegeneration and neuroinflammation. The heterozygous R136S mutation partially protected against APOE4-driven neurodegeneration and neuroinflammation but not Tau pathology. Single-nucleus RNA sequencing revealed that the APOE4-R136S mutation increased disease-protective and diminished disease-associated cell populations in a gene dose-dependent manner. Thus, the APOE-R136S mutation protects against APOE4-driven AD pathologies, providing a target for therapeutic development against AD.
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页码:2104 / 2121
页数:17
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