Integrating personalized gene expression profiles into predictive disease-associated gene pools

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作者
Jörg Menche
Emre Guney
Amitabh Sharma
Patrick J. Branigan
Matthew J. Loza
Frédéric Baribaud
Radu Dobrin
Albert-László Barabási
机构
[1] Northeastern University,Center for Complex Networks Research and Department of Physics
[2] Central European University,Center for Network Science
[3] CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences,Center for Cancer Systems Biology (CCSB) and Department of Cancer Biology
[4] Dana-Farber Cancer Institute,Department of Medicine, Brigham and Womens Hospital
[5] Harvard Medical School,undefined
[6] Janssen Research & Development Inc.,undefined
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摘要
Gene expression data are routinely used to identify genes that on average exhibit different expression levels between a case and a control group. Yet, very few of such differentially expressed genes are detectably perturbed in individual patients. Here, we develop a framework to construct personalized perturbation profiles for individual subjects, identifying the set of genes that are significantly perturbed in each individual. This allows us to characterize the heterogeneity of the molecular manifestations of complex diseases by quantifying the expression-level similarities and differences among patients with the same phenotype. We show that despite the high heterogeneity of the individual perturbation profiles, patients with asthma, Parkinson and Huntington’s disease share a broadpool of sporadically disease-associated genes, and that individuals with statistically significant overlap with this pool have a 80–100% chance of being diagnosed with the disease. The developed framework opens up the possibility to apply gene expression data in the context of precision medicine, with important implications for biomarker identification, drug development, diagnosis and treatment.
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