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Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate

BACKGROUND: The prostate gland is an organ with highly specialized functional attributes that serves to enhance the fertility of mammalian species. Much of the information pertaining to normal and pathological conditions affecting the prostate has been obtained through extensive developmental, bioch...

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Autores principales: Abbott, Denise E, Pritchard, Colin, Clegg, Nigel J, Ferguson, Camari, Dumpit, Ruth, Sikes, Robert A, Nelson, Peter S
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2003
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC329418/
https://www.ncbi.nlm.nih.gov/pubmed/14659016
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author Abbott, Denise E
Pritchard, Colin
Clegg, Nigel J
Ferguson, Camari
Dumpit, Ruth
Sikes, Robert A
Nelson, Peter S
author_facet Abbott, Denise E
Pritchard, Colin
Clegg, Nigel J
Ferguson, Camari
Dumpit, Ruth
Sikes, Robert A
Nelson, Peter S
author_sort Abbott, Denise E
collection PubMed
description BACKGROUND: The prostate gland is an organ with highly specialized functional attributes that serves to enhance the fertility of mammalian species. Much of the information pertaining to normal and pathological conditions affecting the prostate has been obtained through extensive developmental, biochemical and genetic analyses of rodent species. Although important insights can be obtained through detailed anatomical and histological assessments of mouse and rat models, further mechanistic explanations are greatly aided through studies of gene and protein expression. RESULTS: In this article we characterize the repertoire of genes expressed in the normal developing mouse prostate through the analysis of 50,562 expressed sequence tags derived from 14 mouse prostate cDNA libraries. Sequence assemblies and annotations identified 15,009 unique transcriptional units of which more than 600 represent high quality assemblies without corresponding annotations in public gene expression databases. Quantitative analyses demonstrate distinct anatomical and developmental partitioning of prostate gene expression. This finding may assist in the interpretation of comparative studies between human and mouse and guide the development of new transgenic murine disease models. The identification of several novel genes is reported, including a new member of the β-defensin gene family with prostate-restricted expression. CONCLUSIONS: These findings suggest a potential role for the prostate as a defensive barrier for entry of pathogens into the genitourinary tract and, further, serve to emphasize the utility of the continued evaluation of transcriptomes from a diverse repertoire of tissues and cell types.
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spelling pubmed-3294182004-02-05 Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate Abbott, Denise E Pritchard, Colin Clegg, Nigel J Ferguson, Camari Dumpit, Ruth Sikes, Robert A Nelson, Peter S Genome Biol Research BACKGROUND: The prostate gland is an organ with highly specialized functional attributes that serves to enhance the fertility of mammalian species. Much of the information pertaining to normal and pathological conditions affecting the prostate has been obtained through extensive developmental, biochemical and genetic analyses of rodent species. Although important insights can be obtained through detailed anatomical and histological assessments of mouse and rat models, further mechanistic explanations are greatly aided through studies of gene and protein expression. RESULTS: In this article we characterize the repertoire of genes expressed in the normal developing mouse prostate through the analysis of 50,562 expressed sequence tags derived from 14 mouse prostate cDNA libraries. Sequence assemblies and annotations identified 15,009 unique transcriptional units of which more than 600 represent high quality assemblies without corresponding annotations in public gene expression databases. Quantitative analyses demonstrate distinct anatomical and developmental partitioning of prostate gene expression. This finding may assist in the interpretation of comparative studies between human and mouse and guide the development of new transgenic murine disease models. The identification of several novel genes is reported, including a new member of the β-defensin gene family with prostate-restricted expression. CONCLUSIONS: These findings suggest a potential role for the prostate as a defensive barrier for entry of pathogens into the genitourinary tract and, further, serve to emphasize the utility of the continued evaluation of transcriptomes from a diverse repertoire of tissues and cell types. BioMed Central 2003 2003-11-28 /pmc/articles/PMC329418/ /pubmed/14659016 Text en Copyright © 2003 Abbott et al.; licensee BioMed Central Ltd. This is an Open Access article: verbatim copying and redistribution of this article are permitted in all media for any purpose, provided this notice is preserved along with the article's original URL.
spellingShingle Research
Abbott, Denise E
Pritchard, Colin
Clegg, Nigel J
Ferguson, Camari
Dumpit, Ruth
Sikes, Robert A
Nelson, Peter S
Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title_full Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title_fullStr Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title_full_unstemmed Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title_short Expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
title_sort expressed sequence tag profiling identifies developmental and anatomic partitioning of gene expression in the mouse prostate
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC329418/
https://www.ncbi.nlm.nih.gov/pubmed/14659016
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