Author:
Paranjpe Manish D,Belonwu Stella,Wang Jason K,Oskotsky Tomiko,Gupta Aarzu,Taubes Alice,Zalokusky Kelly,Paranjpe Ishan,Glicksberg Benjamin S,Huang Yadong,Sirota Marina,
Abstract
ABSTRACTIn spite of evidence of females having a greater lifetime risk of developing Alzheimer’s Disease (AD) and greater apolipoprotein E4-related (apoE4) AD risk compared to males, molecular signatures underlying these findings remain elusive. We took a meta-analysis approach to study gene expression in the brains of 1,084 AD patients and age-matched controls and whole blood from 645 AD patients and age-matched controls. Gene-expression, network-based analysis and cell type deconvolution approaches revealed a consistent immune signature in the brain and blood of female AD patients that was absent in males. Machine learning-based classification of AD using gene expression from whole blood in addition to clinical features revealed an improvement in classification accuracy upon stratifying by sex, achieving an AUROC of 0.91 for females and 0.80 for males. These results help identify sex and apoE4 genotype-specific transcriptomic signatures of AD and underscore the importance of considering sex in the development of biomarkers and therapeutic strategies for AD.
Publisher
Cold Spring Harbor Laboratory
Cited by
3 articles.
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