A systems genomics approach to uncover patient-specific pathogenic pathways and proteins in a complex disease

Author:

Brooks JohanneORCID,Modos Dezso,Sudhakar Padhmanand,Fazekas David,Zoufir Azedine,Kapuy Orsolya,Szalay-Beko Mate,Madgwick Matthew,Verstockt Bram,Hall Lindsay,Watson Alastair,Tremelling Mark,Parkes Miles,Vermeire Severine,Bender Andreas,Carding Simon R.,Korcsmaros Tamas

Abstract

AbstractWe describe a novel precision medicine workflow, the integrated single nucleotide polymorphism network platform (iSNP), designed to identify the exact mechanisms of how SNPs affect cellular regulatory networks, and how SNP co-occurrences contribute to disease pathogenesis in ulcerative colitis (UC). Using SNP profiles of 377 UC patients, we mapped the regulatory effects of the SNPs to a human signalling network containing protein-protein, miRNA-mRNA and transcription factor binding interactions. Unsupervised clustering algorithms grouped these patient-specific networks into four distinct clusters based on two large disease hubs, NFKB1 and PKCB. Pathway analysis identified the epigenetic modification as common and the T-cell specific responses as differing signalling pathways in the clusters. By integrating individual transcriptomes in active and quiescent disease setting to the patient networks, we validated the impact of non-coding SNPs. The iSNP approach identified regulatory effects of disease-associated non-coding SNPs, and identified how pathogenesis pathways are activated via different genetic modifications.

Publisher

Cold Spring Harbor Laboratory

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