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Identification of Estrogen-responsive Genes Using a Genome-wide Analysis of Promoter Elements for Transcription Factor Binding Sites

We developed a pipeline to identify novel genes regulated by the steroid hormone-dependent transcription factor, estrogen receptor, through a systematic analysis of upstream regions of all human and mouse genes. We built a data base of putative promoter regions for 23,077 human and 19,984 mouse tran...

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Published in:	The Journal of biological chemistry 2005-06, Vol.280 (22), p.21491-21497
Main Authors:	Kamalakaran, Sitharthan, Radhakrishnan, Senthil K., Beck, William T.
Format:	Article
Language:	English
Subjects:	Algorithms Animals Base Sequence Binding Sites Cell Line, Tumor Computational Biology - methods Conserved Sequence CpG Islands Databases, Genetic Dose-Response Relationship, Drug Estrogens - metabolism Genetic Techniques Genome Humans Mice Molecular Sequence Data Promoter Regions, Genetic Protein Binding Receptors, Estrogen - metabolism Response Elements Reverse Transcriptase Polymerase Chain Reaction Software Transcription Factors - metabolism Transcription, Genetic
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cited_by	cdi_FETCH-LOGICAL-c442t-f02fb9d561af626af06d450c24e70c746edfdda9f20b60fe5e6aeacf1e99a17e3
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container_issue	22
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container_title	The Journal of biological chemistry
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creator	Kamalakaran, Sitharthan Radhakrishnan, Senthil K. Beck, William T.
description	We developed a pipeline to identify novel genes regulated by the steroid hormone-dependent transcription factor, estrogen receptor, through a systematic analysis of upstream regions of all human and mouse genes. We built a data base of putative promoter regions for 23,077 human and 19,984 mouse transcripts from National Center for Biotechnology Information annotation and 8793 human and 6785 mouse promoters from the Data Base of Transcriptional Start Sites. We used this data base of putative promoters to identify potential targets of estrogen receptor by identifying estrogen response elements (EREs) in their promoters. Our program correctly identified EREs in genes known to be regulated by estrogen in addition to several new genes whose putative promoters contained EREs. We validated six genes (KIAA1243, NRIP1, MADH9, NME3, TPD52L, and ABCG2) to be estrogen-responsive in MCF7 cells using reverse transcription PCR. To allow for extensibility of our program in identifying targets of other transcription factors, we have built a Web interface to access our data base and programs. Our Web-based program for Promoter Analysis of Genome, PAGen@UIC, allows a user to identify putative target genes for vertebrate transcription factors through the analysis of their upstream sequences. The interface allows the user to search the human and mouse promoter data bases for potential target genes containing one or more listed transcription factor binding sites (TFBSs) in their upstream elements, using either regular expression-based consensus or position weight matrices. The data base can also be searched for promoters harboring user-defined TFBSs given as a consensus or a position weight matrix. Furthermore, the user can retrieve putative promoter sequences for any given gene together with identified TFBSs located on its promoter. Orthologous promoters are also analyzed to determine conserved elements.
doi_str_mv	10.1074/jbc.M409176200
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Our Web-based program for Promoter Analysis of Genome, PAGen@UIC, allows a user to identify putative target genes for vertebrate transcription factors through the analysis of their upstream sequences. The interface allows the user to search the human and mouse promoter data bases for potential target genes containing one or more listed transcription factor binding sites (TFBSs) in their upstream elements, using either regular expression-based consensus or position weight matrices. The data base can also be searched for promoters harboring user-defined TFBSs given as a consensus or a position weight matrix. Furthermore, the user can retrieve putative promoter sequences for any given gene together with identified TFBSs located on its promoter. 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Our Web-based program for Promoter Analysis of Genome, PAGen@UIC, allows a user to identify putative target genes for vertebrate transcription factors through the analysis of their upstream sequences. The interface allows the user to search the human and mouse promoter data bases for potential target genes containing one or more listed transcription factor binding sites (TFBSs) in their upstream elements, using either regular expression-based consensus or position weight matrices. The data base can also be searched for promoters harboring user-defined TFBSs given as a consensus or a position weight matrix. Furthermore, the user can retrieve putative promoter sequences for any given gene together with identified TFBSs located on its promoter. 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subjects	Algorithms Animals Base Sequence Binding Sites Cell Line, Tumor Computational Biology - methods Conserved Sequence CpG Islands Databases, Genetic Dose-Response Relationship, Drug Estrogens - metabolism Genetic Techniques Genome Humans Mice Molecular Sequence Data Promoter Regions, Genetic Protein Binding Receptors, Estrogen - metabolism Response Elements Reverse Transcriptase Polymerase Chain Reaction Software Transcription Factors - metabolism Transcription, Genetic
title	Identification of Estrogen-responsive Genes Using a Genome-wide Analysis of Promoter Elements for Transcription Factor Binding Sites
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