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    Meta-analysis of the Alzheimer's Disease human brain transcriptome and functional dissection in mouse models

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    Authors
    Wan, Y. W.
    Al-Ouran, R.
    Mangleburg, C. G.
    Perumal, T. M.
    Lee, T. V.
    Allison, K.
    Swarup, V.
    Funk, C. C.
    Gaiteri, C.
    Allen, M.
    Wang, M.
    Neuner, S. M.
    Kaczorowski, C. C.
    Philip, V. M.
    Howell, G. R.
    Martini-Stoica, H.
    Zheng, H.
    Mei, H.
    Zhong, X.
    Kim, J. W.
    Dawson, V. L.
    Dawson, T. M.
    Pao, P. C.
    Tsai, L. H.
    Haure-Mirande, J. V.
    Ehrlich, M. E.
    Chakrabarty, P.
    Levites, Y.
    Wang, X.
    Dammer, E. B.
    Srivastava, G.
    Mukherjee, S.
    Sieberts, S. K.
    Omberg, L.
    Dang, K. D.
    Eddy, J. A.
    Snyder, P.
    Chae, Y.
    Amberkar, Sandeep
    Wei, W.
    Hide, W.
    Preuss, C.
    Ergun, A.
    Ebert, P. J.
    Airey, D. C.
    Mostafavi, S.
    Yu, L.
    Klein, H. U.
    Carter, G. W.
    Collier, D. A.
    Golde, T. E.
    Levey, A. I.
    Bennett, D. A.
    Estrada, K.
    Townsend, T. M.
    Zhang, B.
    Schadt, E.
    De Jager, P. L.
    Price, N. D.
    Ertekin-Taner, N.
    Liu, Z.
    Shulman, J. M.
    Mangravite, L. M.
    Logsdon, B. A.
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    Affiliation
    Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX 77030, USA;
    Issue Date
    2020
    
    Metadata
    Show full item record
    Abstract
    We present a consensus atlas of the human brain transcriptome in Alzheimer's disease (AD), based on meta-analysis of differential gene expression in 2,114 postmortem samples. We discover 30 brain coexpression modules from seven regions as the major source of AD transcriptional perturbations. We next examine overlap with 251 brain differentially expressed gene sets from mouse models of AD and other neurodegenerative disorders. Human-mouse overlaps highlight responses to amyloid versus tau pathology and reveal age- and sex-dependent expression signatures for disease progression. Human coexpression modules enriched for neuronal and/or microglial genes broadly overlap with mouse models of AD, Huntington's disease, amyotrophic lateral sclerosis, and aging. Other human coexpression modules, including those implicated in proteostasis, are not activated in AD models but rather following other, unexpected genetic manipulations. Our results comprise a cross-species resource, highlighting transcriptional networks altered by human brain pathophysiology and identifying correspondences with mouse models for AD preclinical studies. Keywords: Alzheimer's disease; RNA-seq; aging; coexpression analysis; differential expression analysis; meta-analysis; mouse models; neuroinflammation; transcriptome.
    Citation
    Wan YW, Al-Ouran R, Mangleburg CG, Perumal TM, Lee TV, Allison K, et al. Meta-Analysis of the Alzheimer's Disease Human Brain Transcriptome and Functional Dissection in Mouse Models. Cell Rep. 2020;32(2):107908.
    Journal
    Cell Reports
    URI
    http://hdl.handle.net/10541/623185
    DOI
    10.1016/j.celrep.2020.107908
    PubMed ID
    32668255
    Additional Links
    https://dx.doi.org/10.1016/j.celrep.2020.107908
    Type
    Article
    Language
    en
    ae974a485f413a2113503eed53cd6c53
    10.1016/j.celrep.2020.107908
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