Multi‐Omics‐Based Autophagy‐Related Untypical Subtypes in Patients with Cerebral Amyloid Pathology

组学 转录组 自噬 计算生物学 蛋白质组学 诱导多能干细胞 生物 载脂蛋白E 神经炎症 代谢组学 生物信息学 疾病 小胶质细胞 系统生物学 神经科学
作者
Jong-Chan Park,Natalia Barahona‐Torres,So‐Young Jang,Kin Y. Mok,Haeng Jun Kim,Sun‐Ho Han,Kwang‐Hyun Cho,Xiaopu Zhou,Amy K. Y. Fu,Nancy Y. Ip,Jieun Seo,Murim Choi,Hyobin Jeong,Daehee Hwang,Dong Young Lee,Min Soo Byun,Dahyun Yi,Jong Won Han,Inhee Mook-Jung,John Hardy
出处
期刊:Advanced Science [Wiley]
卷期号:9 (23): 2201212-2201212
标识
DOI:10.1002/advs.202201212
摘要

Recent multi-omics analyses paved the way for a comprehensive understanding of pathological processes. However, only few studies have explored Alzheimer’s disease (AD) despite the possibility of biological subtypes within these patients. For this study, unsupervised classification of four datasets (genetics, miRNA transcriptomics, proteomics, and blood-based biomarkers) using Multi-Omics Factor Analysis+ (MOFA+), along with systems-biological approaches following various downstream analyses are performed. New subgroups within 170 patients with cerebral amyloid pathology (Aβ+) are revealed and the features of them are identified based on the top-rated targets constructing multi-omics factors of both whole (M-TPAD) and immune-focused models (M-IPAD). The authors explored the characteristics of subtypes and possible key-drivers for AD pathogenesis. Further in-depth studies showed that these subtypes are associated with longitudinal brain changes and autophagy pathways are main contributors. The significance of autophagy or clustering tendency is validated in peripheral blood mononuclear cells (PBMCs; n = 120 including 30 Aβ- and 90 Aβ+), induced pluripotent stem cell-derived human brain organoids/microglia (n = 12 including 5 Aβ-, 5 Aβ+, and CRISPR-Cas9 apolipoprotein isogenic lines), and human brain transcriptome (n = 78). Collectively, this study provides a strategy for precision medicine therapy and drug development for AD using integrative multi-omics analysis and network modelling.

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