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Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice

PURPOSE: Individual differences in patterns of gene expression account for much of the diversity of ocular phenotypes and variation in disease risk. We examined the causes of expression differences, and in their linkage to sequence variants, functional differences, and ocular pathophysiology. METHOD...

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Autores principales: Geisert, Eldon E., Lu, Lu, Freeman-Anderson, Natalie E., Templeton, Justin P., Nassr, Mohamed, Wang, Xusheng, Gu, Weikuan, Jiao, Yan, Williams, Robert W.
Formato: Texto
Lenguaje:English
Publicado: Molecular Vision 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2736153/
https://www.ncbi.nlm.nih.gov/pubmed/19727342
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author Geisert, Eldon E.
Lu, Lu
Freeman-Anderson, Natalie E.
Templeton, Justin P.
Nassr, Mohamed
Wang, Xusheng
Gu, Weikuan
Jiao, Yan
Williams, Robert W.
author_facet Geisert, Eldon E.
Lu, Lu
Freeman-Anderson, Natalie E.
Templeton, Justin P.
Nassr, Mohamed
Wang, Xusheng
Gu, Weikuan
Jiao, Yan
Williams, Robert W.
author_sort Geisert, Eldon E.
collection PubMed
description PURPOSE: Individual differences in patterns of gene expression account for much of the diversity of ocular phenotypes and variation in disease risk. We examined the causes of expression differences, and in their linkage to sequence variants, functional differences, and ocular pathophysiology. METHODS: mRNAs from young adult eyes were hybridized to oligomer microarrays (Affymetrix M430v2). Data were embedded in GeneNetwork with millions of single nucleotide polymorphisms, custom array annotation, and information on complementary cellular, functional, and behavioral traits. The data include male and female samples from 28 common strains, 68 BXD recombinant inbred lines, as well as several mutants and knockouts. RESULTS: We provide a fully integrated resource to map, graph, analyze, and test causes and correlations of differences in gene expression in the eye. Covariance in mRNA expression can be used to infer gene function, extract signatures for different cells or tissues, to define molecular networks, and to map quantitative trait loci that produce expression differences. These data can also be used to connect disease phenotypes with sequence variants. We demonstrate that variation in rhodopsin expression efficiently predicts candidate genes for eight uncloned retinal diseases, including WDR17 for the human RP29 locus. CONCLUSIONS: The high level of strain variation in gene expression is a powerful tool that can be used to explore and test molecular networks underlying variation in structure, function, and disease susceptibility. The integration of these data into GeneNetwork provides users with a workbench to test linkages between sequence differences and eye structure and function.
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spelling pubmed-27361532009-09-02 Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice Geisert, Eldon E. Lu, Lu Freeman-Anderson, Natalie E. Templeton, Justin P. Nassr, Mohamed Wang, Xusheng Gu, Weikuan Jiao, Yan Williams, Robert W. Mol Vis Research Article PURPOSE: Individual differences in patterns of gene expression account for much of the diversity of ocular phenotypes and variation in disease risk. We examined the causes of expression differences, and in their linkage to sequence variants, functional differences, and ocular pathophysiology. METHODS: mRNAs from young adult eyes were hybridized to oligomer microarrays (Affymetrix M430v2). Data were embedded in GeneNetwork with millions of single nucleotide polymorphisms, custom array annotation, and information on complementary cellular, functional, and behavioral traits. The data include male and female samples from 28 common strains, 68 BXD recombinant inbred lines, as well as several mutants and knockouts. RESULTS: We provide a fully integrated resource to map, graph, analyze, and test causes and correlations of differences in gene expression in the eye. Covariance in mRNA expression can be used to infer gene function, extract signatures for different cells or tissues, to define molecular networks, and to map quantitative trait loci that produce expression differences. These data can also be used to connect disease phenotypes with sequence variants. We demonstrate that variation in rhodopsin expression efficiently predicts candidate genes for eight uncloned retinal diseases, including WDR17 for the human RP29 locus. CONCLUSIONS: The high level of strain variation in gene expression is a powerful tool that can be used to explore and test molecular networks underlying variation in structure, function, and disease susceptibility. The integration of these data into GeneNetwork provides users with a workbench to test linkages between sequence differences and eye structure and function. Molecular Vision 2009-08-31 /pmc/articles/PMC2736153/ /pubmed/19727342 Text en http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Geisert, Eldon E.
Lu, Lu
Freeman-Anderson, Natalie E.
Templeton, Justin P.
Nassr, Mohamed
Wang, Xusheng
Gu, Weikuan
Jiao, Yan
Williams, Robert W.
Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title_full Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title_fullStr Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title_full_unstemmed Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title_short Gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
title_sort gene expression in the mouse eye: an online resource for genetics using 103 strains of mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2736153/
https://www.ncbi.nlm.nih.gov/pubmed/19727342
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