Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets

Understanding the gene networks that orchestrate the differentiation of retinal progenitors into photoreceptors in the developing retina is important not only due to its therapeutic applications in treating retinal degeneration but also because the developing retina provides an excellent model for s...

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Main Authors: Laura A. Hecker, Timothy C. Alcon, Vasant G. Honavar, M. Heather West Greenlee
Format: Article
Language:English
Published: SAGE Publishing 2008-01-01
Series:Bioinformatics and Biology Insights
Online Access:https://doi.org/10.4137/BBI.S417
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spelling doaj-f36d06b1c7e8425596c0662bf0acbb512020-11-25T03:17:11ZengSAGE PublishingBioinformatics and Biology Insights1177-93222008-01-01210.4137/BBI.S417Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental TargetsLaura A. Hecker0Timothy C. Alcon1Vasant G. Honavar2M. Heather West Greenlee3 Interdepartmental Neuroscience Program, Iowa State University, Ames, IA 50011. Bioinformatics and Computational Biology Graduate Program, Iowa State University, Ames, IA 50011. Department of Computer Science, Bioinformatics and Computational Biology Graduate Program, Center for Computational Intelligence, Learning and Discovery, Iowa State University, Ames, IA 50011. Department of Biomedical Sciences, Interdepartmental Neuroscience Program, Bioinformatics and Computational Biology Graduate Program, Center for Computational Intelligence, Learning and Discovery, Iowa State University, Ames, IA 50011.Understanding the gene networks that orchestrate the differentiation of retinal progenitors into photoreceptors in the developing retina is important not only due to its therapeutic applications in treating retinal degeneration but also because the developing retina provides an excellent model for studying CNS development. Although several studies have profiled changes in gene expression during normal retinal development, these studies offer at best only a starting point for functional studies focused on a smaller subset of genes. The large number of genes profiled at comparatively few time points makes it extremely difficult to reliably infer gene networks from a gene expression dataset. We describe a novel approach to identify and prioritize from multiple gene expression datasets, a small subset of the genes that are likely to be good candidates for further experimental investigation. We report progress on addressing this problem using a novel approach to querying multiple large-scale expression datasets using a ‘seed network’ consisting of a small set of genes that are implicated by published studies in rod photoreceptor differentiation. We use the seed network to identify and sort a list of genes whose expression levels are highly correlated with those of multiple seed network genes in at least two of the five gene expression datasets. The fact that several of the genes in this list have been demonstrated, through experimental studies reported in the literature, to be important in rod photoreceptor function provides support for the utility of this approach in prioritizing experimental targets for further experimental investigation. Based on Gene Ontology and KEGG pathway annotations for the list of genes obtained in the context of other information available in the literature, we identified seven genes or groups of genes for possible inclusion in the gene network involved in differentiation of retinal progenitor cells into rod photoreceptors. Our approach to querying multiple gene expression datasets using a seed network constructed from known interactions between specific genes of interest provides a promising strategy for focusing hypothesis-driven experiments using large-scale ‘omics’ data.https://doi.org/10.4137/BBI.S417
collection DOAJ
language English
format Article
sources DOAJ
author Laura A. Hecker
Timothy C. Alcon
Vasant G. Honavar
M. Heather West Greenlee
spellingShingle Laura A. Hecker
Timothy C. Alcon
Vasant G. Honavar
M. Heather West Greenlee
Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
Bioinformatics and Biology Insights
author_facet Laura A. Hecker
Timothy C. Alcon
Vasant G. Honavar
M. Heather West Greenlee
author_sort Laura A. Hecker
title Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
title_short Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
title_full Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
title_fullStr Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
title_full_unstemmed Using a Seed-Network to Query Multiple Large-Scale Gene Expression Datasets from the Developing Retina in Order to Identify and Prioritize Experimental Targets
title_sort using a seed-network to query multiple large-scale gene expression datasets from the developing retina in order to identify and prioritize experimental targets
publisher SAGE Publishing
series Bioinformatics and Biology Insights
issn 1177-9322
publishDate 2008-01-01
description Understanding the gene networks that orchestrate the differentiation of retinal progenitors into photoreceptors in the developing retina is important not only due to its therapeutic applications in treating retinal degeneration but also because the developing retina provides an excellent model for studying CNS development. Although several studies have profiled changes in gene expression during normal retinal development, these studies offer at best only a starting point for functional studies focused on a smaller subset of genes. The large number of genes profiled at comparatively few time points makes it extremely difficult to reliably infer gene networks from a gene expression dataset. We describe a novel approach to identify and prioritize from multiple gene expression datasets, a small subset of the genes that are likely to be good candidates for further experimental investigation. We report progress on addressing this problem using a novel approach to querying multiple large-scale expression datasets using a ‘seed network’ consisting of a small set of genes that are implicated by published studies in rod photoreceptor differentiation. We use the seed network to identify and sort a list of genes whose expression levels are highly correlated with those of multiple seed network genes in at least two of the five gene expression datasets. The fact that several of the genes in this list have been demonstrated, through experimental studies reported in the literature, to be important in rod photoreceptor function provides support for the utility of this approach in prioritizing experimental targets for further experimental investigation. Based on Gene Ontology and KEGG pathway annotations for the list of genes obtained in the context of other information available in the literature, we identified seven genes or groups of genes for possible inclusion in the gene network involved in differentiation of retinal progenitor cells into rod photoreceptors. Our approach to querying multiple gene expression datasets using a seed network constructed from known interactions between specific genes of interest provides a promising strategy for focusing hypothesis-driven experiments using large-scale ‘omics’ data.
url https://doi.org/10.4137/BBI.S417
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