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Tissue-specific expression and regulation of sexually dimorphic genes in mice

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Zeitschriftentitel: Genome Research
Personen und Körperschaften: Yang, Xia, Schadt, Eric E., Wang, Susanna, Wang, Hui, Arnold, Arthur P., Ingram-Drake, Leslie, Drake, Thomas A., Lusis, Aldons J.
In: Genome Research, 16, 2006, 8, S. 995-1004
Format: E-Article
Sprache: Englisch
veröffentlicht:
Cold Spring Harbor Laboratory
Schlagwörter:
Genetics (clinical)
Genetics
author_facet Yang, Xia
Schadt, Eric E.
Wang, Susanna
Wang, Hui
Arnold, Arthur P.
Ingram-Drake, Leslie
Drake, Thomas A.
Lusis, Aldons J.
Yang, Xia
Schadt, Eric E.
Wang, Susanna
Wang, Hui
Arnold, Arthur P.
Ingram-Drake, Leslie
Drake, Thomas A.
Lusis, Aldons J.
author Yang, Xia
Schadt, Eric E.
Wang, Susanna
Wang, Hui
Arnold, Arthur P.
Ingram-Drake, Leslie
Drake, Thomas A.
Lusis, Aldons J.
spellingShingle Yang, Xia
Schadt, Eric E.
Wang, Susanna
Wang, Hui
Arnold, Arthur P.
Ingram-Drake, Leslie
Drake, Thomas A.
Lusis, Aldons J.
Genome Research
Tissue-specific expression and regulation of sexually dimorphic genes in mice
Genetics (clinical)
Genetics
author_sort yang, xia
spelling Yang, Xia Schadt, Eric E. Wang, Susanna Wang, Hui Arnold, Arthur P. Ingram-Drake, Leslie Drake, Thomas A. Lusis, Aldons J. 1088-9051 Cold Spring Harbor Laboratory Genetics (clinical) Genetics http://dx.doi.org/10.1101/gr.5217506 <jats:p>We report a comprehensive analysis of gene expression differences between sexes in multiple somatic tissues of 334 mice derived from an intercross between inbred mouse strains C57BL/6J and C3H/HeJ. The analysis of a large number of individuals provided the power to detect relatively small differences in expression between sexes, and the use of an intercross allowed analysis of the genetic control of sexually dimorphic gene expression. Microarray analysis of 23,574 transcripts revealed that the extent of sexual dimorphism in gene expression was much greater than previously recognized. Thus, thousands of genes showed sexual dimorphism in liver, adipose, and muscle, and hundreds of genes were sexually dimorphic in brain. These genes exhibited highly tissue-specific patterns of expression and were enriched for distinct pathways represented in the Gene Ontology database. They also showed evidence of chromosomal enrichment, not only on the sex chromosomes, but also on several autosomes. Genetic analyses provided evidence of the global regulation of subsets of the sexually dimorphic genes, as the transcript levels of a large number of these genes were controlled by several expression quantitative trait loci (eQTL) hotspots that exhibited tissue-specific control. Moreover, many tissue-specific transcription factor binding sites were found to be enriched in the sexually dimorphic genes.</jats:p> Tissue-specific expression and regulation of sexually dimorphic genes in mice Genome Research
doi_str_mv 10.1101/gr.5217506
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title Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_unstemmed Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_full Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_fullStr Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_full_unstemmed Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_short Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_sort tissue-specific expression and regulation of sexually dimorphic genes in mice
topic Genetics (clinical)
Genetics
url http://dx.doi.org/10.1101/gr.5217506
publishDate 2006
physical 995-1004
description <jats:p>We report a comprehensive analysis of gene expression differences between sexes in multiple somatic tissues of 334 mice derived from an intercross between inbred mouse strains C57BL/6J and C3H/HeJ. The analysis of a large number of individuals provided the power to detect relatively small differences in expression between sexes, and the use of an intercross allowed analysis of the genetic control of sexually dimorphic gene expression. Microarray analysis of 23,574 transcripts revealed that the extent of sexual dimorphism in gene expression was much greater than previously recognized. Thus, thousands of genes showed sexual dimorphism in liver, adipose, and muscle, and hundreds of genes were sexually dimorphic in brain. These genes exhibited highly tissue-specific patterns of expression and were enriched for distinct pathways represented in the Gene Ontology database. They also showed evidence of chromosomal enrichment, not only on the sex chromosomes, but also on several autosomes. Genetic analyses provided evidence of the global regulation of subsets of the sexually dimorphic genes, as the transcript levels of a large number of these genes were controlled by several expression quantitative trait loci (eQTL) hotspots that exhibited tissue-specific control. Moreover, many tissue-specific transcription factor binding sites were found to be enriched in the sexually dimorphic genes.</jats:p>
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author Yang, Xia, Schadt, Eric E., Wang, Susanna, Wang, Hui, Arnold, Arthur P., Ingram-Drake, Leslie, Drake, Thomas A., Lusis, Aldons J.
author_facet Yang, Xia, Schadt, Eric E., Wang, Susanna, Wang, Hui, Arnold, Arthur P., Ingram-Drake, Leslie, Drake, Thomas A., Lusis, Aldons J., Yang, Xia, Schadt, Eric E., Wang, Susanna, Wang, Hui, Arnold, Arthur P., Ingram-Drake, Leslie, Drake, Thomas A., Lusis, Aldons J.
author_sort yang, xia
container_issue 8
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container_title Genome Research
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description <jats:p>We report a comprehensive analysis of gene expression differences between sexes in multiple somatic tissues of 334 mice derived from an intercross between inbred mouse strains C57BL/6J and C3H/HeJ. The analysis of a large number of individuals provided the power to detect relatively small differences in expression between sexes, and the use of an intercross allowed analysis of the genetic control of sexually dimorphic gene expression. Microarray analysis of 23,574 transcripts revealed that the extent of sexual dimorphism in gene expression was much greater than previously recognized. Thus, thousands of genes showed sexual dimorphism in liver, adipose, and muscle, and hundreds of genes were sexually dimorphic in brain. These genes exhibited highly tissue-specific patterns of expression and were enriched for distinct pathways represented in the Gene Ontology database. They also showed evidence of chromosomal enrichment, not only on the sex chromosomes, but also on several autosomes. Genetic analyses provided evidence of the global regulation of subsets of the sexually dimorphic genes, as the transcript levels of a large number of these genes were controlled by several expression quantitative trait loci (eQTL) hotspots that exhibited tissue-specific control. Moreover, many tissue-specific transcription factor binding sites were found to be enriched in the sexually dimorphic genes.</jats:p>
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spelling Yang, Xia Schadt, Eric E. Wang, Susanna Wang, Hui Arnold, Arthur P. Ingram-Drake, Leslie Drake, Thomas A. Lusis, Aldons J. 1088-9051 Cold Spring Harbor Laboratory Genetics (clinical) Genetics http://dx.doi.org/10.1101/gr.5217506 <jats:p>We report a comprehensive analysis of gene expression differences between sexes in multiple somatic tissues of 334 mice derived from an intercross between inbred mouse strains C57BL/6J and C3H/HeJ. The analysis of a large number of individuals provided the power to detect relatively small differences in expression between sexes, and the use of an intercross allowed analysis of the genetic control of sexually dimorphic gene expression. Microarray analysis of 23,574 transcripts revealed that the extent of sexual dimorphism in gene expression was much greater than previously recognized. Thus, thousands of genes showed sexual dimorphism in liver, adipose, and muscle, and hundreds of genes were sexually dimorphic in brain. These genes exhibited highly tissue-specific patterns of expression and were enriched for distinct pathways represented in the Gene Ontology database. They also showed evidence of chromosomal enrichment, not only on the sex chromosomes, but also on several autosomes. Genetic analyses provided evidence of the global regulation of subsets of the sexually dimorphic genes, as the transcript levels of a large number of these genes were controlled by several expression quantitative trait loci (eQTL) hotspots that exhibited tissue-specific control. Moreover, many tissue-specific transcription factor binding sites were found to be enriched in the sexually dimorphic genes.</jats:p> Tissue-specific expression and regulation of sexually dimorphic genes in mice Genome Research
spellingShingle Yang, Xia, Schadt, Eric E., Wang, Susanna, Wang, Hui, Arnold, Arthur P., Ingram-Drake, Leslie, Drake, Thomas A., Lusis, Aldons J., Genome Research, Tissue-specific expression and regulation of sexually dimorphic genes in mice, Genetics (clinical), Genetics
title Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_full Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_fullStr Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_full_unstemmed Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_short Tissue-specific expression and regulation of sexually dimorphic genes in mice
title_sort tissue-specific expression and regulation of sexually dimorphic genes in mice
title_unstemmed Tissue-specific expression and regulation of sexually dimorphic genes in mice
topic Genetics (clinical), Genetics
url http://dx.doi.org/10.1101/gr.5217506