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National Institute of Environmental Health Sciences

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Publication Detail

Title: Differential gene regulatory pattern in the human brain from schizophrenia using transcriptomic-causal network.

Authors: Yazdani, Akram; Mendez-Giraldez, Raul; Yazdani, Azam; Kosorok, Michael R; Roussos, Panos

Published In BMC Bioinformatics, (2020 Oct 21)

Abstract: BACKGROUND: Common and complex traits are the consequence of the interaction and regulation of multiple genes simultaneously, therefore characterizing the interconnectivity of genes is essential to unravel the underlying biological networks. However, the focus of many studies is on the differential expression of individual genes or on co-expression analysis. METHODS: Going beyond analysis of one gene at a time, we systematically integrated transcriptomics, genotypes and Hi-C data to identify interconnectivities among individual genes as a causal network. We utilized different machine learning techniques to extract information from the network and identify differential regulatory pattern between cases and controls. We used data from the Allen Brain Atlas for replication. RESULTS: Employing the integrative systems approach on the data from CommonMind Consortium showed that gene transcription is controlled by genetic variants proximal to the gene (cis-regulatory factors), and transcribed distal genes (trans-regulatory factors). We identified differential gene regulatory patterns in SCZ-cases versus controls and novel SCZ-associated genes that may play roles in the disorder since some of them are primary expressed in human brain. In addition, we observed genes known associated with SCZ are not likely (OR = 0.59) to have high impacts (degree > 3) on the network. CONCLUSIONS: Causal networks could reveal underlying patterns and the role of genes individually and as a group. Establishing principles that govern relationships between genes provides a mechanistic understanding of the dysregulated gene transcription patterns in SCZ and creates more efficient experimental designs for further studies. This information cannot be obtained by studying a single gene at the time.

PubMed ID: 33087039 Exiting the NIEHS site

MeSH Terms: No MeSH terms associated with this publication

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