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阿尔茨海默病大规模基因表达图谱表明,运动是最具理论治疗价值的方法。

Alzheimer's disease large-scale gene expression portrait identifies exercise as the top theoretical treatment.

机构信息

Department of Integrative Biology, University of Wisconsin-Madison, Madison, USA.

出版信息

Sci Rep. 2022 Oct 13;12(1):17189. doi: 10.1038/s41598-022-22179-z.

Abstract

Alzheimer's disease (AD) is a complex neurodegenerative disorder that affects multiple brain regions and is difficult to treat. In this study we used 22 AD large-scale gene expression datasets to identify a consistent underlying portrait of AD gene expression across multiple brain regions. Then we used the portrait as a platform for identifying treatments that could reverse AD dysregulated expression patterns. Enrichment of dysregulated AD genes included multiple processes, ranging from cell adhesion to CNS development. The three most dysregulated genes in the AD portrait were the inositol trisphosphate kinase, ITPKB (upregulated), the astrocyte specific intermediate filament protein, GFAP (upregulated), and the rho GTPase, RHOQ (upregulated). 41 of the top AD dysregulated genes were also identified in a recent human AD GWAS study, including PNOC, C4B, and BCL11A. 42 transcription factors were identified that were both dysregulated in AD and that in turn affect expression of other AD dysregulated genes. Male and female AD portraits were highly congruent. Out of over 250 treatments, three datasets for exercise or activity were identified as the top three theoretical treatments for AD via reversal of large-scale gene expression patterns. Exercise reversed expression patterns of hundreds of AD genes across multiple categories, including cytoskeleton, blood vessel development, mitochondrion, and interferon-stimulated related genes. Exercise also ranked as the best treatment across a majority of individual region-specific AD datasets and meta-analysis AD datasets. Fluoxetine also scored well and a theoretical combination of fluoxetine and exercise reversed 549 AD genes. Other positive treatments included curcumin. Comparisons of the AD portrait to a recent depression portrait revealed a high congruence of downregulated genes in both. Together, the AD portrait provides a new platform for understanding AD and identifying potential treatments for AD.

摘要

阿尔茨海默病(AD)是一种复杂的神经退行性疾病,影响多个大脑区域,且难以治疗。在这项研究中,我们使用了 22 个 AD 大规模基因表达数据集,以确定在多个大脑区域中 AD 基因表达的一致潜在特征。然后,我们使用该特征作为平台,以确定可以逆转 AD 失调表达模式的治疗方法。失调的 AD 基因的富集包括多个过程,从细胞粘附到中枢神经系统发育。AD 特征图中最失调的三个基因是肌醇三磷酸激酶,ITPKB(上调),星形胶质细胞特异性中间丝蛋白,GFAP(上调)和 Rho GTPase,RHOQ(上调)。AD 特征图中 41 个最失调的基因也在最近的人类 AD GWAS 研究中被鉴定出来,包括 PNOC,C4B 和 BCL11A。鉴定出 42 个转录因子,它们在 AD 中失调,并且反过来影响其他 AD 失调基因的表达。男性和女性的 AD 特征图高度一致。在 250 多种治疗方法中,有三个数据集确定为运动或活动,是通过逆转大规模基因表达模式来治疗 AD 的前三种理论方法。运动在包括细胞骨架,血管发育,线粒体和干扰素刺激相关基因在内的多个类别中逆转了数百个 AD 基因的表达模式。运动还在大多数个体区域特异性 AD 数据集和荟萃分析 AD 数据集中被评为最佳治疗方法。氟西汀的评分也很高,氟西汀和运动的理论组合逆转了 549 个 AD 基因。其他积极的治疗方法包括姜黄素。将 AD 特征图与最近的抑郁症特征图进行比较,发现两者下调的基因高度一致。总之,AD 特征图为理解 AD 和确定 AD 的潜在治疗方法提供了一个新的平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a32a/9561721/42f4b3e55423/41598_2022_22179_Fig1_HTML.jpg

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