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  <title>BibSonomy publications for /bibtex/2807a67270a546f62bfff708ba1566444/marcoalvarez</title>
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  <dc:date>2008-09-05T08:27:51+02:00</dc:date>

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<item rdf:about="http://www.bibsonomy.org/uri/bibtex/2807a67270a546f62bfff708ba1566444/marcoalvarez">
    <title>Identifying transcription factor binding sites through markov chain optimization</title>
    <link>http://www.bibsonomy.org/bibtex/2807a67270a546f62bfff708ba1566444/marcoalvarez</link>
    <dc:creator>marcoalvarez</dc:creator>
    <dc:date>2008-05-14T11:33:59+02:00</dc:date>
    <dc:subject>Markov TFBS </dc:subject>
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  <a href="http://www.bibsonomy.org/bibtex/2807a67270a546f62bfff708ba1566444/marcoalvarez">Identifying transcription factor binding sites through markov chain optimization</a>
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<div class="bmdesc">
  <span style="color:#555555;"> 
    Kyle <a href="http://www.bibsonomy.org/author/Ellrott">Ellrott</a>         	     	 
        	  and Chuhu <a href="http://www.bibsonomy.org/author/Yang">Yang</a>         	     	 
        	  and Frances M. <a href="http://www.bibsonomy.org/author/Sladek">Sladek</a>         	     	 
        	  and Tao <a href="http://www.bibsonomy.org/author/Jiang">Jiang</a>         	     	 
        	 </span> 
  <em>Bioinformatics</em>
      <b>18</b>
      S100--S109
  (2002)
</div>
<span class="bmmeta">
  
  
        to
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        <a href="http://www.bibsonomy.org/user/marcoalvarez/Markov">Markov</a>
        <a href="http://www.bibsonomy.org/user/marcoalvarez/TFBS">TFBS</a>
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        on 2008-05-14 11:33:59 </span></div>
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        <swrc:journal>Bioinformatics</swrc:journal><swrc:number>Suppl. 2</swrc:number><swrc:pages>S100--S109</swrc:pages><swrc:title>Identifying transcription factor binding sites through markov chain
	optimization</swrc:title><swrc:volume>18</swrc:volume><swrc:year>2002</swrc:year><swrc:keywords>Markov TFBS </swrc:keywords><swrc:date>2008-05-14 11:33:59.0</swrc:date><swrc:abstract>Even though every cell in an organism contains the same genetic material,
	each cell does not express the same cohort of genes. Therefore, one
	of the major problems facing genomic research today is to determine
	not only which genes are differentially expressed and under what
	conditions, but also how the expression of those genes is regulated.
	The first step in determining differential gene expression is the
	binding of sequence-specific DNA binding proteins (i.e. transcription
	factors) to regulatory regions of the genes (i.e. promoters and enhancers).
	An important aspect to understanding how a given transcription factor
	functions is to know the entire gamut of binding sites and subsequently
	potential target genes that the factor may bind/regulate. In this
	study, we have developed a computer algorithm to scan genomic databases
	for transcription factor binding sites, based on a novel Markov chain
	optimization method, and used it to scan the human genome for sites
	that bind to hepatocyte nuclear factor 4 alpha (HNF4alpha). A list
	of 71 known HNF4alpha binding sites from the literature were used
	to train our Markov chain model. By looking at the window of 600
	nucleotides around the transcription start site of each confirmed
	gene on the human genome, we identified 849 sites with varying binding
	potential and experimentally tested 109 of those sites for binding
	to HNF4alpha. Our results show that the program was very successful
	in identifying 77 new HNF4alpha binding sites with varying binding
	affinities (i.e. a 71\% success rate). Therefore, this computational
	method for searching genomic databases for potential transcription
	factor binding sites is a powerful tool for investigating mechanisms
	of differential gene regulation.</swrc:abstract><swrc:author>
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  <rdf:_2><swrc:Person swrc:name="Chuhu Yang" /></rdf:_2>
  <rdf:_3><swrc:Person swrc:name="Frances M. Sladek" /></rdf:_3>
  <rdf:_4><swrc:Person swrc:name="Tao Jiang" /></rdf:_4>
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