阿尔茨海默病的综合多模态细胞图谱。
Integrated multimodal cell atlas of Alzheimer's disease.
作者信息
Gabitto Mariano I, Travaglini Kyle J, Rachleff Victoria M, Kaplan Eitan S, Long Brian, Ariza Jeanelle, Ding Yi, Mahoney Joseph T, Dee Nick, Goldy Jeff, Melief Erica J, Agrawal Anamika, Kana Omar, Zhen Xingjian, Barlow Samuel T, Brouner Krissy, Campos Jazmin, Campos John, Carr Ambrose J, Casper Tamara, Chakrabarty Rushil, Clark Michael, Cool Jonah, Dalley Rachel, Darvas Martin, Ding Song-Lin, Dolbeare Tim, Egdorf Tom, Esposito Luke, Ferrer Rebecca, Fleckenstein Lynn E, Gala Rohan, Gary Amanda, Gelfand Emily, Gloe Jessica, Guilford Nathan, Guzman Junitta, Hirschstein Daniel, Ho Windy, Hupp Madison, Jarsky Tim, Johansen Nelson, Kalmbach Brian E, Keene Lisa M, Khawand Sarah, Kilgore Mitchell D, Kirkland Amanda, Kunst Michael, Lee Brian R, Leytze Mckaila, Mac Donald Christine L, Malone Jocelin, Maltzer Zoe, Martin Naomi, McCue Rachel, McMillen Delissa, Mena Gonzalo, Meyerdierks Emma, Meyers Kelly P, Mollenkopf Tyler, Montine Mark, Nolan Amber L, Nyhus Julie K, Olsen Paul A, Pacleb Maiya, Pagan Chelsea M, Peña Nicholas, Pham Trangthanh, Pom Christina Alice, Postupna Nadia, Rimorin Christine, Ruiz Augustin, Saldi Giuseppe A, Schantz Aimee M, Shapovalova Nadiya V, Sorensen Staci A, Staats Brian, Sullivan Matt, Sunkin Susan M, Thompson Carol, Tieu Michael, Ting Jonathan T, Torkelson Amy, Tran Tracy, Valera Cuevas Nasmil J, Walling-Bell Sarah, Wang Ming-Qiang, Waters Jack, Wilson Angela M, Xiao Ming, Haynor David, Gatto Nicole M, Jayadev Suman, Mufti Shoaib, Ng Lydia, Mukherjee Shubhabrata, Crane Paul K, Latimer Caitlin S, Levi Boaz P, Smith Kimberly A, Close Jennie L, Miller Jeremy A, Hodge Rebecca D, Larson Eric B, Grabowski Thomas J, Hawrylycz Michael, Keene C Dirk, Lein Ed S
机构信息
Allen Institute for Brain Science, Seattle, WA, USA.
Department of Statistics, University of Washington, Seattle, WA, USA.
出版信息
Nat Neurosci. 2024 Dec;27(12):2366-2383. doi: 10.1038/s41593-024-01774-5. Epub 2024 Oct 14.
Alzheimer's disease (AD) is the leading cause of dementia in older adults. Although AD progression is characterized by stereotyped accumulation of proteinopathies, the affected cellular populations remain understudied. Here we use multiomics, spatial genomics and reference atlases from the BRAIN Initiative to study middle temporal gyrus cell types in 84 donors with varying AD pathologies. This cohort includes 33 male donors and 51 female donors, with an average age at time of death of 88 years. We used quantitative neuropathology to place donors along a disease pseudoprogression score. Pseudoprogression analysis revealed two disease phases: an early phase with a slow increase in pathology, presence of inflammatory microglia, reactive astrocytes, loss of somatostatin inhibitory neurons, and a remyelination response by oligodendrocyte precursor cells; and a later phase with exponential increase in pathology, loss of excitatory neurons and Pvalb and Vip inhibitory neuron subtypes. These findings were replicated in other major AD studies.
阿尔茨海默病(AD)是老年人痴呆的主要原因。尽管AD的进展以蛋白病变的刻板积累为特征,但受影响的细胞群体仍未得到充分研究。在这里,我们使用来自大脑计划的多组学、空间基因组学和参考图谱,研究了84名具有不同AD病理的供体的颞中回细胞类型。该队列包括33名男性供体和51名女性供体,死亡时的平均年龄为88岁。我们使用定量神经病理学将供体按照疾病假进展评分进行分类。假进展分析揭示了两个疾病阶段:早期病理缓慢增加,存在炎性小胶质细胞、反应性星形胶质细胞、生长抑素抑制性神经元丧失,以及少突胶质细胞前体细胞的髓鞘再生反应;后期病理呈指数增加,兴奋性神经元以及Pvalb和Vip抑制性神经元亚型丧失。这些发现已在其他主要的AD研究中得到重复。
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