TY - JOUR
T1 - B-cell ligand processing pathways detected by large-scale comparative analysis
AU - Towfic, Fadi
AU - Gupta, Shakti
AU - Honavar, Vasant
AU - Subramaniam, Shankar
N1 - Funding Information:
This research was supported in part by a Cornette Fellowship award and an Integrative Graduate Education and Research Training (IGERT) fellowship to FT, funded by the National Science Foundation (NSF) Grant ( DGE 0504304 ) to Iowa State University and NSF Grants 0939370 , 0835541 and 0641037 awarded to SS. We also thank Raj Srikrishnan for his help in data processing. The work of VH was supported by the NSF, while working at the Foundation. Any opinion, finding, and conclusions contained in this article are those of the authors and do not necessarily reflect the views of the National Science Foundation.
PY - 2012/6
Y1 - 2012/6
N2 - The initiation of B-cell ligand recognition is a critical step for the generation of an immune response against foreign bodies. We sought to identify the biochemical pathways involved in the B-cell ligand recognition cascade and sets of ligands that trigger similar immunological responses. We utilized several comparative approaches to analyze the gene coexpression networks generated from a set of microarray experiments spanning 33 different ligands. First, we compared the degree distributions of the generated networks. Second, we utilized a pairwise network alignment algorithm, BiNA, to align the networks based on the hubs in the networks. Third, we aligned the networks based on a set of KEGG pathways. We summarized our results by constructing a consensus hierarchy of pathways that are involved in B cell ligand recognition. The resulting pathways were further validated through literature for their common physiological responses. Collectively, the results based on our comparative analyses of degree distributions, alignment of hubs, and alignment based on KEGG pathways provide a basis for molecular characterization of the immune response states of B-cells and demonstrate the power of comparative approaches (e.g., gene coexpression network alignment algorithms) in elucidating biochemical pathways involved in complex signaling events in cells.
AB - The initiation of B-cell ligand recognition is a critical step for the generation of an immune response against foreign bodies. We sought to identify the biochemical pathways involved in the B-cell ligand recognition cascade and sets of ligands that trigger similar immunological responses. We utilized several comparative approaches to analyze the gene coexpression networks generated from a set of microarray experiments spanning 33 different ligands. First, we compared the degree distributions of the generated networks. Second, we utilized a pairwise network alignment algorithm, BiNA, to align the networks based on the hubs in the networks. Third, we aligned the networks based on a set of KEGG pathways. We summarized our results by constructing a consensus hierarchy of pathways that are involved in B cell ligand recognition. The resulting pathways were further validated through literature for their common physiological responses. Collectively, the results based on our comparative analyses of degree distributions, alignment of hubs, and alignment based on KEGG pathways provide a basis for molecular characterization of the immune response states of B-cells and demonstrate the power of comparative approaches (e.g., gene coexpression network alignment algorithms) in elucidating biochemical pathways involved in complex signaling events in cells.
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U2 - 10.1016/j.gpb.2012.03.001
DO - 10.1016/j.gpb.2012.03.001
M3 - Article
C2 - 22917187
AN - SCOPUS:84865345841
SN - 1672-0229
VL - 10
SP - 142
EP - 152
JO - Genomics, Proteomics and Bioinformatics
JF - Genomics, Proteomics and Bioinformatics
IS - 3
ER -