Literature DB >> 21070623

Discovering hidden relationships between renal diseases and regulated genes through 3D network visualizations.

Suresh K Bhavnani1, Arunkumaar Ganesan, Theodore Hall, Eric Maslowski, Felix Eichinger, Sebastian Martini, Paul Saxman, Gowtham Bellala, Matthias Kretzler.   

Abstract

BACKGROUND: In a recent study, two-dimensional (2D) network layouts were used to visualize and quantitatively analyze the relationship between chronic renal diseases and regulated genes. The results revealed complex relationships between disease type, gene specificity, and gene regulation type, which led to important insights about the underlying biological pathways. Here we describe an attempt to extend our understanding of these complex relationships by reanalyzing the data using three-dimensional (3D) network layouts, displayed through 2D and 3D viewing methods.
FINDINGS: The 3D network layout (displayed through the 3D viewing method) revealed that genes implicated in many diseases (non-specific genes) tended to be predominantly down-regulated, whereas genes regulated in a few diseases (disease-specific genes) tended to be up-regulated. This new global relationship was quantitatively validated through comparison to 1000 random permutations of networks of the same size and distribution. Our new finding appeared to be the result of using specific features of the 3D viewing method to analyze the 3D renal network.
CONCLUSIONS: The global relationship between gene regulation and gene specificity is the first clue from human studies that there exist common mechanisms across several renal diseases, which suggest hypotheses for the underlying mechanisms. Furthermore, the study suggests hypotheses for why the 3D visualization helped to make salient a new regularity that was difficult to detect in 2D. Future research that tests these hypotheses should enable a more systematic understanding of when and how to use 3D network visualizations to reveal complex regularities in biological networks.

Entities:  

Year:  2010        PMID: 21070623      PMCID: PMC3001742          DOI: 10.1186/1756-0500-3-296

Source DB:  PubMed          Journal:  BMC Res Notes        ISSN: 1756-0500


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