Discovering transnosological molecular basis of human brain diseases using biclustering analysis of integrated gene expression data

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Background: It has been reported that several brain diseases can be treated as transnosological manner implicating possible common molecular basis under those diseases. However, molecular level commonality among those brain diseases has been largely unexplored. Gene expression analyses of human brain have been used to find genes associated with brain diseases but most of those studies were restricted either to an individual disease or to a couple of diseases. In addition, identifying significant genes in such brain diseases mostly failed when it used typical methods depending on differentially expressed genes. Results: In this study, we used a correlation-based biclustering approach to find coexpressed gene sets in five neurodegenerative diseases and three psychiatric disorders. By using biclustering analysis, we could efficiently and fairly identified various gene sets expressed specifically in both single and multiple brain diseases. We could find 4,307 gene sets correlatively expressed in multiple brain diseases and 3,409 gene sets exclusively specified in individual brain diseases. The function enrichment analysis of those gene sets showed many new possible functional bases as well as neurological processes that are common or specific for those eight diseases. Conclusions: This study introduces possible common molecular bases for several brain diseases, which open the opportunity to clarify the transnosological perspective assumed in brain diseases. It also showed the advantages of correlation-based biclustering analysis and accompanying function enrichment analysis for gene expression data in this type of investigation.
Publisher
BIOMED CENTRAL LTD
Issue Date
2015-05
Language
English
Article Type
Article
Keywords

MICROARRAY ANALYSIS; TRANSCRIPTOME; KNOWLEDGE; PATHOLOGY; CANCER

Citation

BMC MEDICAL INFORMATICS AND DECISION MAKING, v.15

ISSN
1472-6947
DOI
10.1186/1472-6947-15-S1-S7
URI
http://hdl.handle.net/10203/206013
Appears in Collection
BiS-Journal Papers(저널논문)
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