transfic_web: transFIC_web/transFIC

comparison transFIC_web/transFIC_web.xml @ 4:7e8b135145d0 draft default tip

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author	saketkc
date	Tue, 15 Apr 2014 13:05:23 -0400
parents	4051693fb690
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-:4051693fb690
+:7e8b135145d0
 <tool id="transFIC_web" name="TransFIC">
 <description>TransFIC web service</description>
+<requirements>
+<requirement type="package" version="2.2.1">requests</requirement>
+<requirement type="package" version="7.19.3.1">pycurl</requirement>
+<requirement type="package" version="4.1.0">beautifulsoup4</requirement>
+<requirement type="python-module">requests</requirement>
+<requirement type="python-package">pycurl</requirement>
+<requirement type="python-package">bs4</requirement>
+</requirements>
 <command interpreter="python">
 transFIC_web.py --input $input --output $output
 </command>
 <inputs>
 <param name="input" format="text" type="data" label="Inout Variants"/>
 <outputs>
 <data name="output" format="tabular"/>
 </outputs>
 <tests>
 <test>
-<param name="input" value="condel_input.txt"/>
+<param name="input" value="condel_input.tsv"/>
 <output name="output" file="transfic_output.csv"/>
 </test>
 </tests>
+<help>
+**What it does**
+This script calls TransFIC web api at  http://bg.upf.edu/transfic/
+TransFIC stands for TRANsformed Functional Impact for Cancer.
+It is a method to transform Functional Impact Scores taking into account the differences in basal tolerance to germline SNVs of genes that belong to
+different functional classes. This transformation allows to use the scores provided by well-known tools (e.g. SIFT, Polyphen2, MutationAssessor)
+to rank the functional impact of cancer somatic mutations. Mutations with greater transFIC are more likely to be cancer drivers.
+**How does it work**
+TransFIC takes as input the Functional Impact Score of a somatic mutation provided by one of the aforementioned tools.
+It then compares that score to the distribution of scores of germline SNVs observed in genes with similar functional
+annotations (for instance genes with the same molecular function as provided by the Gene Ontologies).
+The score is thus transformed using the Zscore formula.
+The result is that mutations in genes that are less tolerant to germline SNVs are amplified,
+while the scores of mutations on relatively tolerant genes are decreased.
+**Input**
+There are two main formats allowed:
+SNVs may be submitted for analysis both in chromosome and protein coordinates.
+The chromosome coordinates (hg19) input must follow this format:
+[CHROMOSOME] [START] [END] [MUTANT_NUCLEOTIDE]
+The END column is the same as the START for SNVs.
+Those four columns must be separated by tabs. Also a fifth column can optionally be added with the Variant name
+Ex:
+9   32473058    32473058    A
+7   43918688    43918688    C
+Additionally, the input could be composed by two columns the strand of the SNV and an identifier:
+[PROTEIN_ID][variant]
+Also tab separated. Currently only Uniprot, RefSeq_Peptide and Ensembl identifiers are recognized by the webserver.
+The variant column must contain the following information (in this order ): change_position, reference_aminoacid and changed_aminoacid
+**Citation**
+If you use this Galaxy tool in work leading to a scientific publication please cite:
+Gonzalez-Perez A, Deu-Pons J and Lopez-Bigas N. Improving the prediction of the functional impact of cancer mutations by baseline tolerance transformation
+Genome Medicine 2012. 4:89 doi:10.1186/gm390s
+</help>
 </tool>

Mercurial > repos > saketkc > transfic_web

comparison transFIC_web/transFIC_web.xml @ 4:7e8b135145d0 draft default tip