Readhead Benjamin P, Mastroeni Diego F, Wang Qi, Sierra Maria A, de Ávila Camila, Jimoh Tajudeen O, Haure-Mirande Jean-Vianney, Atanasoff Kristina E, Nolz Jennifer, Suazo Crystal, Barton Nathaniel J, Orszulak Adrian R, Chigas Samantha M, Tran Khanh, Mirza Anne, Ryon Krista, Proszynski Jacqueline, Najjar Deena, Dudley Joel T, Liu Sean T H, Gandy Sam, Ehrlich Michelle E, Alsop Eric, Antone Jerry, Reiman Rebecca, Funk Cory, Best Rebecca L, Jhatro Michael, Kamath Kathy, Shon John, Kowalik Timothy F, Bennett David A, Liang Winnie S, Serrano Geidy E, Beach Thomas G, Van Keuren-Jensen Kendall, Mason Christopher E, Chan Yingleong, Lim Elaine T, Tortorella Domenico, Reiman Eric M
ASU-Banner Neurodegenerative Disease Research Center, Arizona State University, Tempe, Arizona, USA.
Department of Physiology and Biophysics, Weill Cornell Medicine, New York, New York, USA.
Alzheimers Dement. 2025 Jan;21(1):e14401. doi: 10.1002/alz.14401. Epub 2024 Dec 19.
While there may be microbial contributions to Alzheimer's disease (AD), findings have been inconclusive. We recently reported an AD-associated CD83(+) microglia subtype associated with increased immunoglobulin G4 (IgG4) in the transverse colon (TC).
We used immunohistochemistry (IHC), IgG4 repertoire profiling, and brain organoid experiments to explore this association.
CD83(+) microglia in the superior frontal gyrus (SFG) are associated with elevated IgG4 and human cytomegalovirus (HCMV) in the TC, anti-HCMV IgG4 in cerebrospinal fluid, and both HCMV and IgG4 in the SFG and vagal nerve. This association was replicated in an independent AD cohort. HCMV-infected cerebral organoids showed accelerated AD pathophysiological features (Aβ42 and pTau-212) and neuronal death.
Findings indicate complex, cross-tissue interactions between HCMV and the adaptive immune response associated with CD83(+) microglia in persons with AD. This may indicate an opportunity for antiviral therapy in persons with AD and biomarker evidence of HCMV, IgG4, or CD83(+) microglia.
Cross-tissue interaction between HCMV and the adaptive immune response in a subset of persons with AD. Presence of CD83(+) microglial associated with IgG4 and HCMV in the gut. CD83(+) microglia are also associated presence of HCMV and IgG4 in the cortex and vagal nerve. Replication of key association in an independent cohort of AD subjects. HCMV infection of cerebral organoids accelerates the production of AD neuropathological features.
虽然微生物可能与阿尔茨海默病(AD)有关,但其研究结果尚无定论。我们最近报告了一种与AD相关的CD83(+)小胶质细胞亚型,其与横结肠(TC)中免疫球蛋白G4(IgG4)的增加有关。
我们使用免疫组织化学(IHC)、IgG4库分析和脑类器官实验来探究这种关联。
额上回(SFG)中的CD83(+)小胶质细胞与TC中IgG4和人巨细胞病毒(HCMV)水平升高、脑脊液中抗HCMV IgG4以及SFG和迷走神经中的HCMV和IgG4均相关。这种关联在一个独立的AD队列中得到了重复验证。感染HCMV的脑类器官表现出加速的AD病理生理特征(Aβ42和pTau-212)以及神经元死亡。
研究结果表明,在AD患者中,HCMV与与CD83(+)小胶质细胞相关的适应性免疫反应之间存在复杂的跨组织相互作用。这可能为AD患者以及有HCMV、IgG4或CD83(+)小胶质细胞生物标志物证据的患者提供抗病毒治疗的机会。
AD患者亚群中HCMV与适应性免疫反应之间的跨组织相互作用。肠道中存在与IgG4和HCMV相关的CD83(+)小胶质细胞。CD83(+)小胶质细胞也与皮质和迷走神经中HCMV和IgG4的存在相关。在一个独立的AD受试者队列中重复了关键关联。脑类器官的HCMV感染加速了AD神经病理特征的产生。
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