An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease

Microarray-based profiling represents an effective method to analyze cellular or tissue-specific gene expression on the genome-level. However, in comparative analyses between control and mutant samples, microarrays often identify a large number of differentially expressed genes, in turn making it ch...

Descripción completa

Detalles Bibliográficos
Autores principales: Anand, Deepti, Agrawal, Smriti A., Siddam, Archana D., Motohashi, Hozumi, Yamamoto, Masayuki, Lachke, Salil A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Data in Brief
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4500531/
https://www.ncbi.nlm.nih.gov/pubmed/26185746
http://dx.doi.org/10.1016/j.gdata.2015.06.017
_version_ 1782380927059492864
author Anand, Deepti
Agrawal, Smriti A.
Siddam, Archana D.
Motohashi, Hozumi
Yamamoto, Masayuki
Lachke, Salil A.
author_facet Anand, Deepti
Agrawal, Smriti A.
Siddam, Archana D.
Motohashi, Hozumi
Yamamoto, Masayuki
Lachke, Salil A.
author_sort Anand, Deepti
collection PubMed
description Microarray-based profiling represents an effective method to analyze cellular or tissue-specific gene expression on the genome-level. However, in comparative analyses between control and mutant samples, microarrays often identify a large number of differentially expressed genes, in turn making it challenging to isolate the select “high-priority candidates” that are most relevant to an observed mutant phenotype. Here, we describe an integrative approach for mouse mutant lens microarray gene expression analysis using publically accessible systems-level information such as wild-type mouse lens expression data in iSyTE (integrated Systems Tool for Eye gene discovery), protein–protein interaction data in public databases, gene ontology enrichment data, and transcription factor binding profile data. This strategy, when applied to small Maf Mafg −/−:Mafk +/− mouse lens microarray datasets (deposited in NCBI Gene Expression Omnibus database with accession number GSE65500) in Agrawal et al. 2015 [1], led to the effective prioritization of candidate genes linked to lens defects in these mutants. Indeed, from the original list of genes that are differentially expressed at ± 1.5-fold and p < 0.05 in Mafg −/−:Mafk +/− mutant lenses, this analysis led to the identification of thirty-six high-priority candidates, in turn reducing the number of genes for further study by approximately 1/3 of the total. Moreover, eight of these genes are linked to mammalian cataract in the published literature, validating the efficacy of this approach. Additionally, these high-priority candidates contribute valuable information for the assembly of a gene regulatory network in the lens. In sum, the pipeline outlined in this report represents an effective approach for initial as well as downstream microarray expression data analysis to identify genes important for lens biology and cataracts. We anticipate that this integrative strategy can be extended to prioritize phenotypically relevant candidate genes from microarray data in other cells and tissues.
format Online
Article
Text
id pubmed-4500531
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-45005312015-10-19 An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease Anand, Deepti Agrawal, Smriti A. Siddam, Archana D. Motohashi, Hozumi Yamamoto, Masayuki Lachke, Salil A. Genom Data Data in Brief Microarray-based profiling represents an effective method to analyze cellular or tissue-specific gene expression on the genome-level. However, in comparative analyses between control and mutant samples, microarrays often identify a large number of differentially expressed genes, in turn making it challenging to isolate the select “high-priority candidates” that are most relevant to an observed mutant phenotype. Here, we describe an integrative approach for mouse mutant lens microarray gene expression analysis using publically accessible systems-level information such as wild-type mouse lens expression data in iSyTE (integrated Systems Tool for Eye gene discovery), protein–protein interaction data in public databases, gene ontology enrichment data, and transcription factor binding profile data. This strategy, when applied to small Maf Mafg −/−:Mafk +/− mouse lens microarray datasets (deposited in NCBI Gene Expression Omnibus database with accession number GSE65500) in Agrawal et al. 2015 [1], led to the effective prioritization of candidate genes linked to lens defects in these mutants. Indeed, from the original list of genes that are differentially expressed at ± 1.5-fold and p < 0.05 in Mafg −/−:Mafk +/− mutant lenses, this analysis led to the identification of thirty-six high-priority candidates, in turn reducing the number of genes for further study by approximately 1/3 of the total. Moreover, eight of these genes are linked to mammalian cataract in the published literature, validating the efficacy of this approach. Additionally, these high-priority candidates contribute valuable information for the assembly of a gene regulatory network in the lens. In sum, the pipeline outlined in this report represents an effective approach for initial as well as downstream microarray expression data analysis to identify genes important for lens biology and cataracts. We anticipate that this integrative strategy can be extended to prioritize phenotypically relevant candidate genes from microarray data in other cells and tissues. Elsevier 2015-06-14 /pmc/articles/PMC4500531/ /pubmed/26185746 http://dx.doi.org/10.1016/j.gdata.2015.06.017 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Data in Brief
Anand, Deepti
Agrawal, Smriti A.
Siddam, Archana D.
Motohashi, Hozumi
Yamamoto, Masayuki
Lachke, Salil A.
An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title_full An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title_fullStr An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title_full_unstemmed An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title_short An integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
title_sort integrative approach to analyze microarray datasets for prioritization of genes relevant to lens biology and disease
topic Data in Brief
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4500531/
https://www.ncbi.nlm.nih.gov/pubmed/26185746
http://dx.doi.org/10.1016/j.gdata.2015.06.017
work_keys_str_mv AT ananddeepti anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT agrawalsmritia anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT siddamarchanad anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT motohashihozumi anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT yamamotomasayuki anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT lachkesalila anintegrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT ananddeepti integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT agrawalsmritia integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT siddamarchanad integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT motohashihozumi integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT yamamotomasayuki integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease
AT lachkesalila integrativeapproachtoanalyzemicroarraydatasetsforprioritizationofgenesrelevanttolensbiologyanddisease

Ejemplares similares