Integrating explainable artificial intelligence with multiomics systems biology and electronic health record data mining for personalized drug repurposing in Alzheimer’s disease

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Mottaqi2025Integrating-CCBYNC.pdf (2.34 MB)
Date
2025
Authors
Mottaqi, Mohammadsadeq
Zhang, Pengyue
Xie, Lei
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American English
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Biostatistics and Health Data Science, Richard M. Fairbanks School of Public Health
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Oxford University Press
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Abstract

Alzheimer's disease (AD) is characterized by region- and patient-specific molecular heterogeneity, which hinders therapeutic design. In this study, we introduce PRISM-ML (PRecision-medicine using Interpretable Systems and Multiomics with Machine Learning), an open-source integrated analysis pipeline that combines interpretable machine learning with systems biology and electronic health records data mining to elucidate the molecular diversity of AD and predict promising drug repurposing opportunities. First, we integrated and harmonized transcriptomic (bulk RNA-seq) and genomic (genome-wide association study) data from 2105 brain samples, each with matched data from the same individual (1363 AD patients, 742 controls; 9 tissues), sourced from three independent studies. Random forest classifiers with SHapley Additive exPlanations identified patient-specific biomarkers; unsupervised clustering resolved 36 molecularly distinct subtissues (defined as clusters of samples within a brain tissue that share a specific expression pattern); and gene-gene coexpression networks prioritized 262 high-centrality bottleneck genes as putative regulators of dysregulated pathways. Next, knowledge graph-based drug repurposing predicted six Food and Drug Administration (FDA)-approved drugs that simultaneously target multiple bottleneck genes and multiple AD-relevant pathways. Notably, in a large US de-identified insurance-claims database (n = 364 733), exposure to promethazine, one of the candidate drugs, was associated with a 57%-62% lower incidence of AD versus an active antihistamine comparator (adjusted hazard ratio 0.38; inverse-probability weighted 0.43; both P < .001), providing real-world support for its repurposing potential. In summary, PRISM-ML, as an explainable multiomics analysis pipeline, is readily transferable to other complex diseases, advancing precision medicine.

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Machine learning, Computational biology, GWAS, Transcriptomics, Personalized medicine, Electronic health records
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Cite As
Mottaqi M, Zhang P, Xie L. Integrating explainable artificial intelligence with multiomics systems biology and electronic health record data mining for personalized drug repurposing in Alzheimer's disease. Brief Bioinform. 2025;26(6):bbaf623. doi:10.1093/bib/bbaf623
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Briefings in Bioinformatics
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Attribution-NonCommercial 4.0 International Creative Commons licenses
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PMC
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https://hdl.handle.net/1805/52503
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https://doi.org/10.1093/bib/bbaf623
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Final published version
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