阿尔茨海默病各阶段的转录模式具有细胞类型特异性,并与人类酒精使用障碍的影响部分趋同。

IF 2.7 3区 医学 Q3 NEUROSCIENCES eNeuro Pub Date : 2024-10-16 Print Date: 2024-10-01 DOI:10.1523/ENEURO.0118-24.2024
Arpita Joshi, Federico Manuel Giorgi, Pietro Paolo Sanna
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引用次数: 0

摘要

单细胞技术的进步促进了新脑细胞类型的发现和表征,进而有助于更好地了解阿尔茨海默病(AD)的发病机制。在这里,我们详细分析了颞中回(MTG)三个阶段的单核(sn)RNA-seq数据,并将其与酒精使用障碍(AUD)患者前额叶皮层的snRNA-seq数据进行了比较。我们观察到抑制性和兴奋性神经元均明显减少,这与之前的报道基本一致。我们观察到几种细胞类型特定的基因表达和通路失调,这些基因表达和通路失调可划分出 AD 的不同阶段。内皮细胞和血管脑膜细胞(VLMCs)的基因表达变化程度最大。神经变性的细胞类型特异性证据可见于多种神经元细胞类型,尤其是 SST(体生长抑素)和 L5 ET(5 层延脑外)神经元等。非神经元细胞中出现了炎症反应的证据,尤其是在中晚期 AD 中。我们观察到AD和AUD中存在共同的扰动,尤其是在转录、翻译、细胞凋亡、自噬、钙信号转导、神经炎症和磷酸化等通路中,这意味着存在共同的转录致病机制,并支持酒精摄入过量在AD进展中的作用。主要的 AUD 基因标记物形成并扰乱了与中晚期 AD 显著相关的基因网络。对AUD基因标记物的主调节因子分析显示,在智力障碍、神经炎症和其他神经退行性疾病中具有影响的转录因子与晚期AD有显著相关性,这进一步表明AD和AUD之间存在共同的转录变化关系。通过分析新皮质中与阿尔茨海默病进展相关的转录变化,并将其与酒精中毒性精神障碍的转录变化进行比较,我们揭示了这两种疾病之间共同的基因表达和通路失调。我们的研究结果证实了之前关于神经元耗竭的研究,并突出了对AD阶段细胞类型特异性基因表达模式的新见解。此外,共同遗传特征的确定表明,AUD 可能会加剧 AD 的进展。这项全面的分析不仅加深了我们对AD病理的了解,还强调了将AUD视为加速AD发病或严重程度的潜在风险因素的重要性。
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Transcriptional Patterns in Stages of Alzheimer's Disease Are Cell-Type-Specific and Partially Converge with the Effects of Alcohol Use Disorder in Humans.

Advances in single-cell technologies have led to the discovery and characterization of new brain cell types, which in turn lead to a better understanding of the pathogenesis of Alzheimer's disease (AD). Here, we present a detailed analysis of single-nucleus (sn)RNA-seq data for three stages of AD from middle temporal gyrus and compare it with snRNA-seq data from the prefrontal cortices from individuals with alcohol use disorder (AUD). We observed a significant decrease in both inhibitory and excitatory neurons, in general agreement with previous reports. We observed several cell-type-specific gene expressions and pathway dysregulations that delineate AD stages. Endothelial and vascular leptomeningeal cells showed the greatest degree of gene expression changes. Cell-type-specific evidence of neurodegeneration was seen in multiple neuronal cell types particularly in somatostatin and Layer 5 extratelencephalic neurons, among others. Evidence of inflammatory responses was seen in non-neuronal cells, particularly in intermediate and advanced AD. We observed common perturbations in AD and AUD, particularly in pathways, like transcription, translation, apoptosis, autophagy, calcium signaling, neuroinflammation, and phosphorylation, that imply shared transcriptional pathogenic mechanisms and support the role of excessive alcohol intake in AD progression. Major AUD gene markers form and perturb a network of genes significantly associated with intermediate and advanced AD. Master regulator analysis from AUD gene markers revealed significant correlation with advanced AD of transcription factors that have implications in intellectual disability, neuroinflammation, and other neurodegenerative conditions, further suggesting a shared nexus of transcriptional changes between AD and AUD.

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来源期刊
eNeuro
eNeuro Neuroscience-General Neuroscience
CiteScore
5.00
自引率
2.90%
发文量
486
审稿时长
16 weeks
期刊介绍: An open-access journal from the Society for Neuroscience, eNeuro publishes high-quality, broad-based, peer-reviewed research focused solely on the field of neuroscience. eNeuro embodies an emerging scientific vision that offers a new experience for authors and readers, all in support of the Society’s mission to advance understanding of the brain and nervous system.
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