Using blood transcriptome analysis for Alzheimer's disease diagnosis and patient stratification

Author:

Zhong Huan12,Zhou Xiaopu123,Uhm Hyebin1,Jiang Yuanbing12,Cao Han1,Chen Yu134,Mak Tiffany T. W.12,Lo Ronnie Ming Nok1,Wong Bonnie Wing Yan12,Cheng Elaine Yee Ling12,Mok Kin Y.125,Chan Andrew Lung Tat6,Kwok Timothy C. Y.7,Mok Vincent C. T.8,Ip Fanny C. F.123,Hardy John259,Fu Amy K. Y.123,Ip Nancy Y.123ORCID

Affiliation:

1. Division of Life Science State Key Laboratory of Molecular Neuroscience and Molecular Neuroscience Center The Hong Kong University of Science and Technology HKSAR China

2. Hong Kong Center for Neurodegenerative Diseases InnoHK HKSAR China

3. Guangdong Provincial Key Laboratory of Brain Science Disease and Drug Development HKUST Shenzhen Research Institute Shenzhen Guangdong China

4. The Brain Cognition and Brain Disease Institute Shenzhen Institutes of Advanced Technology Chinese Academy of Sciences Shenzhen–Hong Kong Institute of Brain Science‐Shenzhen Fundamental Research Institutions Shenzhen Guangdong China

5. Department of Neurodegenerative Disease UCL Institute of Neurology London UK

6. Department of Medicine Queen Elizabeth Hospital HKSAR China

7. Therese Pei Fong Chow Research Centre for Prevention of Dementia Division of Geriatrics Department of Medicine and Therapeutics The Chinese University of Hong Kong HKSAR China

8. Lau Tat‐chuen Research Centre of Brain Degenerative Diseases in Chinese Therese Pei Fong Chow Research Centre for Prevention of Dementia Gerald Choa Neuroscience Institute Li Ka Shing Institute of Health Sciences Division of Neurology Department of Medicine and Therapeutics The Chinese University of Hong Kong HKSAR China

9. Institute for Advanced Study The Hong Kong University of Science and Technology HKSAR China

Abstract

AbstractINTRODUCTIONBlood protein biomarkers demonstrate potential for Alzheimer's disease (AD) diagnosis. Limited studies examine the molecular changes in AD blood cells.METHODSBulk RNA‐sequencing of blood cells was performed on AD patients of Chinese descent (n = 214 and 26 in the discovery and validation cohorts, respectively) with normal controls (n = 208 and 38 in the discovery and validation cohorts, respectively). Weighted gene co‐expression network analysis (WGCNA) and deconvolution analysis identified AD‐associated gene modules and blood cell types. Regression and unsupervised clustering analysis identified AD‐associated genes, gene modules, cell types, and established AD classification models.RESULTSWGCNA on differentially expressed genes revealed 15 gene modules, with 6 accurately classifying AD (areas under the receiver operating characteristics curve [auROCs] > 0.90). These modules stratified AD patients into subgroups with distinct disease states. Cell‐type deconvolution analysis identified specific blood cell types potentially associated with AD pathogenesis.DISCUSSIONThis study highlights the potential of blood transcriptome for AD diagnosis, patient stratification, and mechanistic studies.Highlights We comprehensively analyze the blood transcriptomes of a well‐characterized Alzheimer's disease cohort to identify genes, gene modules, pathways, and specific blood cells associated with the disease. Blood transcriptome analysis accurately classifies and stratifies patients with Alzheimer's disease, with some gene modules achieving classification accuracy comparable to that of the plasma ATN biomarkers. Immune‐associated pathways and immune cells, such as neutrophils, have potential roles in the pathogenesis and progression of Alzheimer's disease.

Publisher

Wiley

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