Mercurial > repos > peterjc > tmhmm_and_signalp
view tools/protein_analysis/psortb.xml @ 15:6abd809cefdd draft
Uploaded v0.2.4, added unit tests for Promoter 2
author | peterjc |
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date | Thu, 25 Apr 2013 12:25:52 -0400 |
parents | 99b82a2b1272 |
children | 7de64c8b258d |
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<tool id="Psortb" name="psortb" version="0.0.1"> <description>Determines sub-cellular localisation of bacterial/archaeal protein sequences</description> <!-- If job splitting is enabled, break up the query file into parts --> <!-- Using 2000 chunks meaning 4 threads doing 500 each is ideal --> <parallelism method="basic" split_inputs="fasta_file" split_mode="to_size" split_size="2000" merge_outputs="tabular_file"></parallelism> <version_command interpreter="python">psortb.py --version</version_command> <command interpreter="python">psortb.py "\$NSLOTS" "$type" "$long" "$cutoff" "$divergent" "$sequence" "$outfile"</command> <stdio> <!-- Anything other than zero is an error --> <exit_code range="1:" /> <exit_code range=":-1" /> </stdio> <inputs> <param format="fasta" name="sequence" type="data" label="Input sequences for which to predict localisation (protein FASTA format)" /> <param name="type" type="select" label="Organism type (N.B. all sequences in the above file must be of the same type)" > <option value="-p">Gram positive bacteria</option> <option value="-n">Gram negative bacteria</option> <option value="-a">Archaea</option> </param> <param name="long" type="select" label="Output type"> <option value="terse">Short (terse, tabular with 3 columns)</option> <!-- The normal output is text, not tabular - worth offering? <option value="normal">Normal</option> --> <option value="long">Long (verbose, tabular with about 30 columns, depending on organism type)</option> </param> <param name="cutoff" size="10" type="float" optional="true" value="" label="Sets a cutoff value for reported results (e.g. 7.5)" help="Leave blank or use zero for no cutoff." /> <param name="divergent" size="10" type="float" optional="true" value="" label="Sets a cutoff value for the multiple localization flag (e.g. 4.5)" help="Leave blank or use zero for no cutoff." /> </inputs> <outputs> <data format="tabular" name="outfile" /> </outputs> <requirements> <requirement type="binary">psort</requirement> </requirements> <tests> <test> <param name="sequence" value="empty.fasta" ftype="fasta"/> <param name="long" value="terse"/> <output name="outfile" file="empty_psortb_terse.tabular" ftype="tabular"/> </test> <test> <param name="sequence" value="k12_ten_proteins.fasta" ftype="fasta"/> <param name="long" value="terse"/> <output name="outfile" file="k12_ten_proteins_psortb_p_terse.tabular" ftype="tabular"/> </test> </tests> <help> **What it does** This calls the command line tool PSORTb v3.0 for prediction of prokaryotic localization sites. The input dataset needs to be protein FASTA sequences. The default output is a simple tabular file with three columns, one row per query sequence: ====== ============================== Column Description ------ ------------------------------ 1 Sequence identifier 2 Localisation, e.g. Cytoplasmic 3 Score ====== ============================== The long output is also tabular with one row per query sequence, but has lots more columns (a different set for each supported organism type). In both cases, a simple header line is included (starting with a hash, #, so that Galaxy treats it as a comment) giving the column names. **References** N.Y. Yu, J.R. Wagner, M.R. Laird, G. Melli, S. Rey, R. Lo, P. Dao, S.C. Sahinalp, M. Ester, L.J. Foster, F.S.L. Brinkman (2010) PSORTb 3.0: Improved protein subcellular localization prediction with refined localization subcategories and predictive capabilities for all prokaryotes, Bioinformatics 26(13):1608-1615 http://dx.doi.org/10.1093/bioinformatics/btq249 http://www.psort.org/documentation/index.html </help> </tool>