Difference between revisions of "Msigdb v2 release notes"

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<br />Details on how the gene set databases were generated is provided below:<br /><br />
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<a href="http://www.broad.mit.edu/gsea/">GSEA Home</a> |  <a href="../../software/software_index.html">Software</a> | <a href="../../msigdb/msigdb_index.html">MSigDB</a> | [[Main_Page|Documentation]] | <a href="../../resources/resources_index.html">Resources</a>  <br />
 +
<br />
 +
Details on how the gene set databases were generated is provided below:<br />
 +
<br />
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C1 (Positional gene sets)</span></h3>
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C1 (Positional gene sets)</span></h3>
Cytogenetic locations were parsed from hugo (October 2006) and Unigene(build 197). When there were conflicts, the Unigene entry was used.<br /><br />
+
Cytogenetic locations were parsed from hugo (October 2006) and Unigene(build 197). When there were conflicts, the Unigene entry was used.<br />
 +
<br />
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C2 (Curated gene sets)</span></h3>
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C2 (Curated gene sets)</span></h3>
 
C2 sets were curated from several sources including:<br />
 
C2 sets were curated from several sources including:<br />
 
<p class="MsoNormal" style="line-height: 150%;">  </p>
 
<p class="MsoNormal" style="line-height: 150%;">  </p>
<em style=""><u><span style="font-family: Arial;">Online pathway databases</span></u></em><em style=""><span style="font-family: Arial;">: </span></em>Several online resources provide catalogs of well studied metabolic and signaling pathways as well as functional categories of genes. We downloaded gene sets from 12 such databases into our system.<br /><br />
+
<em style=""><u><span style="font-family: Arial;">Online pathway databases</span></u></em><em style=""><span style="font-family: Arial;">: </span></em>Several online resources provide catalogs of well studied metabolic and signaling pathways as well as functional categories of genes. We downloaded gene sets from 12 such databases into our system.<br />
 +
<br />
 
<table cellspacing="0" cellpadding="0" border="1" class="MsoTableGrid" style="border: medium none ; border-collapse: collapse; width: 872px; height: 602px;">
 
<table cellspacing="0" cellpadding="0" border="1" class="MsoTableGrid" style="border: medium none ; border-collapse: collapse; width: 872px; height: 602px;">
 
     <tbody>
 
     <tbody>
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         </tr>
 
         </tr>
 
         <tr style="height: 13.2pt;">
 
         <tr style="height: 13.2pt;">
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 13.2pt;">BioCarta<br /></td>
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             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 13.2pt;">BioCarta<br />
 +
            </td>
 
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 13.2pt;">                          [http://www.biocarta.com http://www.biocarta.com]</td>
 
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 13.2pt;">                          [http://www.biocarta.com http://www.biocarta.com]</td>
 
         </tr>
 
         </tr>
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         <tr style="height: 14.25pt;">
 
         <tr style="height: 14.25pt;">
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 14.25pt;">                          Signaling gateway</td>
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 14.25pt;">                          Signaling gateway</td>
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 14.25pt;">[http://www.signaling-gateway.org/ http://www.signaling-gateway.org/]<br /></td>
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             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 14.25pt;">[http://www.signaling-gateway.org/ http://www.signaling-gateway.org/]<br />
 +
            </td>
 
         </tr>
 
         </tr>
 
         <tr style="height: 27.45pt;">
 
         <tr style="height: 27.45pt;">
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         <tr style="height: 13.2pt;">
 
         <tr style="height: 13.2pt;">
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 13.2pt;">                          GenMAPP</td>
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 13.2pt;">                          GenMAPP</td>
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 13.2pt;">[http://www.genmapp.org/ http://www.genmapp.org/]<br /></td>
+
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 13.2pt;">[http://www.genmapp.org/ http://www.genmapp.org/]<br />
 +
            </td>
 
         </tr>
 
         </tr>
 
         <tr style="height: 14.25pt;">
 
         <tr style="height: 14.25pt;">
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         <tr style="height: 27.45pt;">
 
         <tr style="height: 27.45pt;">
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 27.45pt;">                          Human cancer genome anatomy consortium</td>
 
             <td width="271" valign="top" style="border-style: none solid solid; border-color: -moz-use-text-color windowtext windowtext; border-width: medium 1pt 1pt; padding: 0in 5.4pt; width: 203.4pt; height: 27.45pt;">                          Human cancer genome anatomy consortium</td>
             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 27.45pt;">&nbsp;[http://cgap.nci.nih.gov/<br />&nbsp;http://cgap.nci.nih.gov/]</td>
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             <td width="374" valign="top" style="border-style: none solid solid none; border-color: -moz-use-text-color windowtext windowtext -moz-use-text-color; border-width: medium 1pt 1pt medium; padding: 0in 5.4pt; width: 280.3pt; height: 27.45pt;">&nbsp;[http://cgap.nci.nih.gov/<br />
 +
            &nbsp;http://cgap.nci.nih.gov/]</td>
 
         </tr>
 
         </tr>
 
         <tr style="height: 13.2pt;">
 
         <tr style="height: 13.2pt;">
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<br />
 
<br />
 
<p class="MsoNormal" style="line-height: 150%;">  </p>
 
<p class="MsoNormal" style="line-height: 150%;">  </p>
<em style=""><u><span style="font-family: Arial;"><br />Biomedical literature</span></u></em><em style=""><span style="font-family: Arial;">: </span></em><span style="font-family: Arial;">Over the past few years, microarray studies have identified signatures of several important biological and clinical states (e.g. cancer metastasis, stem cell characteristics, drug resistance). These gene sets are valuable biological results. Unfortunately, because gene sets are typically published as tables in a paper, the </span><span style="line-height: 150%; font-family: Arial;">important biological findings they represent are not easily accessible to computational tools. Our first goal was to convert published gene sets into an electronic form. Towards this we compiled a list of microarray articles with published gene expression signatures. From each article, we extracted one or more gene set from tables in the main text or supplementary information. Notably, our focus was on capturing the identity (e.g. gene symbol, GenBank accession) of all members in a gene set rather than on relationships between individual genes. </span><span style="font-family: Arial;">Currently the process of curating a gene set from the literature is largely manual. In this report we include a collection of 1181 gene sets curated in this manner from 343 distinct PubMed accessions.</span><span style="line-height: 150%; font-family: Arial;"></span> <br /><br /><span style="font-weight: bold;"></span>
+
<em style=""><u><span style="font-family: Arial;"><br />
 
+
Biomedical literature</span></u></em><em style=""><span style="font-family: Arial;">: </span></em><span style="font-family: Arial;">Over the past few years, microarray studies have identified signatures of several important biological and clinical states (e.g. cancer metastasis, stem cell characteristics, drug resistance). These gene sets are valuable biological results. Unfortunately, because gene sets are typically published as tables in a paper, the </span><span style="line-height: 150%; font-family: Arial;">important biological findings they represent are not easily accessible to computational tools. Our first goal was to convert published gene sets into an electronic form. Towards this we compiled a list of microarray articles with published gene expression signatures. From each article, we extracted one or more gene set from tables in the main text or supplementary information. Notably, our focus was on capturing the identity (e.g. gene symbol, GenBank accession) of all members in a gene set rather than on relationships between individual genes. </span><span style="font-family: Arial;">Currently the process of curating a gene set from the literature is largely manual. In this report we include a collection of 1181 gene sets curated in this manner from 343 distinct PubMed accessions.</span> <br />
 +
<br />
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C3 (sequence motif gene sets)</span></h3>
 
<h3><span style="font-weight: bold; color: rgb(255, 0, 0);">C3 (sequence motif gene sets)</span></h3>
<p class="MsoNormal" style="line-height: 150%;"><span style="font-weight: bold; color: rgb(255, 0, 0);"></span><span style="font-family: Arial; color: black;">We compiled gene sets on the basis of<span style="">&nbsp; </span>shared regulatory motifs from a recently published comparative analysis of the Human, Mouse, Rat and Dog genomes </span><!--[if supportFields]><span
+
<p class="MsoNormal" style="line-height: 150%;"><span style="font-family: Arial; color: black;">We compiled gene sets on the basis of<span style="">&nbsp; </span>shared regulatory motifs from a recently published comparative analysis of the Human, Mouse, Rat and Dog genomes </span><!--[if supportFields]><span
 
style='font-family:Arial;color:black'><span style='mso-element:field-begin'></span><span
 
style='font-family:Arial;color:black'><span style='mso-element:field-begin'></span><span
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
+
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Xie&lt;/Author&gt;&lt;Year&gt;2005&lt;/Year&gt;&lt;RecNum&gt;342&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Xie&lt;/Author&gt;&lt;Year&gt;2005&lt;/Year&gt;&lt;RecNum&gt;342&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
name='genesets_db.enl' path='C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl'&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
 
name='genesets_db.enl' path='C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl'&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
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</span>&lt;/style&gt;&lt;/url&gt;&lt;/related-urls&gt;&lt;/urls&gt;&lt;/record&gt;&lt;/Cite&gt;&lt;/EndNote&gt;<span
 
</span>&lt;/style&gt;&lt;/url&gt;&lt;/related-urls&gt;&lt;/urls&gt;&lt;/record&gt;&lt;/Cite&gt;&lt;/EndNote&gt;<span
 
style='mso-element:field-separator'></span></span><![endif]--><span style="font-family: Arial; color: black;">(Xie, Lu et al. 2005)</span><!--[if supportFields]><span
 
style='mso-element:field-separator'></span></span><![endif]--><span style="font-family: Arial; color: black;">(Xie, Lu et al. 2005)</span><!--[if supportFields]><span
style='font-family:Arial;color:black'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial; color: black;">. This database consists of 837 motifs sets including 222 microRNA target gene sets.<br /></span></p>
+
style='font-family:Arial;color:black'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial; color: black;">. This database consists of 837 motifs sets including 222 microRNA target gene sets.<br />
<h3><span style="font-family: Arial; color: black;"><span style="font-weight: bold; color: rgb(255, 0, 0);">C4 (computed gene sets)</span></span><span style="font-family: Arial;"></span></h3>
+
</span></p>
 +
<h3><span style="font-family: Arial; color: black;"><span style="font-weight: bold; color: rgb(255, 0, 0);">C4 (computed gene sets)</span></span></h3>
 
<p><span style="font-family: Arial;">We mined 4 expression compendia datasets for correlated gene sets by searching for neighbors (i.e. genes with similar expression profiles across a compendium) of <span style="">&nbsp;</span>380 cancer associated genes </span><!--[if supportFields]><span
 
<p><span style="font-family: Arial;">We mined 4 expression compendia datasets for correlated gene sets by searching for neighbors (i.e. genes with similar expression profiles across a compendium) of <span style="">&nbsp;</span>380 cancer associated genes </span><!--[if supportFields]><span
 
style='font-family:Arial'><span style='mso-element:field-begin'></span><span
 
style='font-family:Arial'><span style='mso-element:field-begin'></span><span
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
+
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Brentani&lt;/Author&gt;&lt;Year&gt;2003&lt;/Year&gt;&lt;RecNum&gt;184&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Brentani&lt;/Author&gt;&lt;Year&gt;2003&lt;/Year&gt;&lt;RecNum&gt;184&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
name='genesets_db.enl' path='C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl'&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
 
name='genesets_db.enl' path='C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl'&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
Line 437: Line 448:
 
style='font-family:Arial'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial;">. Neighborhoods with &lt;25 genes at a Pearson correlation threshold of 0.8 were omitted yielding 427 sets. This category of the database is identical to that previously reported in <span style="">&nbsp;</span></span><!--[if supportFields]><span
 
style='font-family:Arial'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial;">. Neighborhoods with &lt;25 genes at a Pearson correlation threshold of 0.8 were omitted yielding 427 sets. This category of the database is identical to that previously reported in <span style="">&nbsp;</span></span><!--[if supportFields]><span
 
style='font-family:Arial'><span style='mso-element:field-begin'></span><span
 
style='font-family:Arial'><span style='mso-element:field-begin'></span><span
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
+
style='mso-spacerun:yes'> </span>ADDIN EN.CITE
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Subramanian&lt;/Author&gt;&lt;Year&gt;2005&lt;/Year&gt;&lt;RecNum&gt;369&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
&lt;EndNote&gt;&lt;Cite&gt;&lt;Author&gt;Subramanian&lt;/Author&gt;&lt;Year&gt;2005&lt;/Year&gt;&lt;RecNum&gt;369&lt;/RecNum&gt;&lt;record&gt;&lt;database
 
name=&quot;genesets_db.enl&quot; path=&quot;C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl&quot;&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
 
name=&quot;genesets_db.enl&quot; path=&quot;C:\Local\xdev\active\msigdb\DOC_PUSH\genesets_db.enl&quot;&gt;genesets_db.enl&lt;/database&gt;&lt;source-app
Line 494: Line 505:
 
face=&quot;normal&quot; font=&quot;default&quot;
 
face=&quot;normal&quot; font=&quot;default&quot;
 
size=&quot;100%&quot;&gt;http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&amp;amp;db=PubMed&amp;amp;dopt=Citation&amp;amp;list_uids=16199517<span
 
size=&quot;100%&quot;&gt;http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&amp;amp;db=PubMed&amp;amp;dopt=Citation&amp;amp;list_uids=16199517<span
style='mso-spacerun:yes'>  </span>&lt;/style&gt;&lt;/url&gt;&lt;/related-urls&gt;&lt;/urls&gt;&lt;/record&gt;&lt;/Cite&gt;&lt;/EndNote&gt;<span
+
style='mso-spacerun:yes'> </span>&lt;/style&gt;&lt;/url&gt;&lt;/related-urls&gt;&lt;/urls&gt;&lt;/record&gt;&lt;/Cite&gt;&lt;/EndNote&gt;<span
 
style='mso-element:field-separator'></span></span><![endif]--><span style="font-family: Arial;">(Subramanian, Tamayo et al. 2005)</span><!--[if supportFields]><span
 
style='mso-element:field-separator'></span></span><![endif]--><span style="font-family: Arial;">(Subramanian, Tamayo et al. 2005)</span><!--[if supportFields]><span
 
style='font-family:Arial'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial;">.</span></p>
 
style='font-family:Arial'><span style='mso-element:field-end'></span></span><![endif]--><span style="font-family: Arial;">.</span></p>

Revision as of 11:15, 23 January 2007

<a href="http://www.broad.mit.edu/gsea/">GSEA Home</a> | <a href="../../software/software_index.html">Software</a> | <a href="../../msigdb/msigdb_index.html">MSigDB</a> | Documentation | <a href="../../resources/resources_index.html">Resources</a>

Details on how the gene set databases were generated is provided below:

C1 (Positional gene sets)

Cytogenetic locations were parsed from hugo (October 2006) and Unigene(build 197). When there were conflicts, the Unigene entry was used.

C2 (Curated gene sets)

C2 sets were curated from several sources including:

Online pathway databases: Several online resources provide catalogs of well studied metabolic and signaling pathways as well as functional categories of genes. We downloaded gene sets from 12 such databases into our system.

<tbody> </tbody>

Name

URL/Reference

BioCarta
http://www.biocarta.com
Signaling pathway database http://www.grt.kyushu-u.ac.jp/spad/menu.html
Signaling gateway http://www.signaling-gateway.org/
Signal transduction knowledge environment http://stke.sciencemag.org/
Human protein reference database http://www.hprd.org/
GenMAPP http://www.genmapp.org/
KEGG http://www.genome.jp/kegg/
Gene ontology http://www.geneontology.org
Sigma-Aldrich pathways http://www.sigmaaldrich.com/Area_of_Interest/Biochemicals/Enzyme_Explorer/Key_Resources.html
Gene arrays, BioScience Corp http://www.superarray.com/
Human cancer genome anatomy consortium  [http://cgap.nci.nih.gov/
 http://cgap.nci.nih.gov/]
NetAffx http://www.affymetrix.com/index.affx



Biomedical literature
: Over the past few years, microarray studies have identified signatures of several important biological and clinical states (e.g. cancer metastasis, stem cell characteristics, drug resistance). These gene sets are valuable biological results. Unfortunately, because gene sets are typically published as tables in a paper, the important biological findings they represent are not easily accessible to computational tools. Our first goal was to convert published gene sets into an electronic form. Towards this we compiled a list of microarray articles with published gene expression signatures. From each article, we extracted one or more gene set from tables in the main text or supplementary information. Notably, our focus was on capturing the identity (e.g. gene symbol, GenBank accession) of all members in a gene set rather than on relationships between individual genes. Currently the process of curating a gene set from the literature is largely manual. In this report we include a collection of 1181 gene sets curated in this manner from 343 distinct PubMed accessions.

C3 (sequence motif gene sets)

We compiled gene sets on the basis of  shared regulatory motifs from a recently published comparative analysis of the Human, Mouse, Rat and Dog genomes (Xie, Lu et al. 2005). This database consists of 837 motifs sets including 222 microRNA target gene sets.

C4 (computed gene sets)

We mined 4 expression compendia datasets for correlated gene sets by searching for neighbors (i.e. genes with similar expression profiles across a compendium) of  380 cancer associated genes (Brentani, Caballero et al. 2003). Neighborhoods with <25 genes at a Pearson correlation threshold of 0.8 were omitted yielding 427 sets. This category of the database is identical to that previously reported in  (Subramanian, Tamayo et al. 2005).