Mercurial > repos > gregory-minevich > bcftools_view
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| author | gregory-minevich |
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| date | Mon, 08 Oct 2012 16:12:40 -0400 |
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<tool id="bcftools_view" name="bcftools view" version="0.0.1"> <description>Converts BCF format to VCF format</description> <requirements> <requirements type="package">samtools</requirements> </requirements> <command interpreter="python"> bcftools_view.py bcftools view #if str( $A ) == "true": -A #end if #if str( $b ) == "true": -b #end if #if $D.seq_dictionary == "true": -D "$D.input" #end if #if str( $F ) == "true": -F #end if #if str( $G ) == "true": -G #end if #if str( $N ) == "true": -N #end if #if str( $S ) == "true": -S #end if #if str( $u) == "true": -u #end if #if str( $c ) == "true": -c #end if #if str( $e ) == "true": -e #end if #if str( $g ) == "true": -g #end if #if $i.alt_indel_snp_ratio == "true": -i $i.ratio #end if #if $p.variant_filter == "true": -p $p.float_value #end if #if $t.mutation_rate == "true": -t $t.rate #end if #if str( $v ) == "true": -v #end if $input > $output </command> <inputs> <param name="input" type="data" format="bcf" label="Choose a bcf file to view" /> <param name="A" type="select" label="Retain all possible alternate alleles at variant sites"> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="b" type="select" label="Output in the BCF format. The default is VCF."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <conditional name="D"> <param name="seq_dictionary" type="select" label="Sequence dictionary (list of chromosome names) for VCF->BCF conversion."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <when value="true"> <param name="input" type="data" format="tabular" label="Sequence dictionary" /> </when> </conditional> <param name="F" type="select" label="Indicate PL is generated by r921 or before (ordering is different)."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="G" type="select" label="Suppress all individual genotype information."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="N" type="select" label="Skip sites where the REF field is not A/C/G/T"> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="S" type="select" label="The input is VCF instead of BCF."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="u" type="select" label="Uncompressed BCF output."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="c" type="select" label="Call variants using Bayesian inference. Automatically performs max-likelihood inference only"> <option value="true" selected="true">Yes</option> <option value="false">No</option> </param> <param name="e" type="select" label="Perform max-likelihood inference only, including estimating the site allele frequency, testing Hardy-Weinberg equilibrium and testing associations with LRT."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <param name="g" type="select" label="Call per-sample genotypes at variant sites"> <option value="true" selected="true">Yes</option> <option value="false">No</option> </param> <conditional name="i"> <param name="alt_indel_snp_ratio" type="select" label="Use alternate INDEL-to-SNP mutation rate, default 0.15."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <when value="true"> <param name="ratio" type="float" label="Ratio (float)" value="0.15" /> </when> </conditional> <conditional name="p"> <param name="variant_filter" type="select" > <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <when value="true"> <param name="float_value" type="float" label="Float" value="0.5" /> </when> </conditional> <conditional name="t"> <param name="mutation_rate" type="select" label="Specify scaled mutation rate for variant calling, default is 0.001."> <option value="true">Yes</option> <option value="false" selected="true">No</option> </param> <when value="true"> <param name="rate" type="float" label="Mutation Rate (float)" value="0.001" /> </when> </conditional> <param name="v" type="select" label="Output variant sites only."> <option value="true" selected="true">Yes</option> <option value="false">No</option> </param> </inputs> <outputs> <data format="tabular" name="output" /> </outputs> <help> **What it does:** This tool converts BCF files into VCF files using BCFtools view from the SAMtools set of utilities: http://samtools.sourceforge.net/samtools.shtml#4 ------ **Citation:** For the underlying tool, please cite `Li H, Handsaker B, Wysoker A, Fennell T, Ruan J, Homer N, Marth G, Abecasis G, Durbin R; 1000 Genome Project Data Processing Subgroup. The Sequence Alignment/Map format and SAMtools. Bioinformatics. 2009 Aug 15;25(16):2078-9. <http://www.ncbi.nlm.nih.gov/pubmed/19505943>`_ If you use this tool within Galaxy, please cite `Gregory Minevich, Danny S. Park, Daniel Blankenberg, Richard J. Poole, and Oliver Hobert. CloudMap: A Cloud-based Pipeline for Analysis of Mutant Genome Sequences. (Genetics 2012 In Press)`__ .. __: http://biochemistry.hs.columbia.edu/labs/hobert/literature.html Correspondence to gm2123@columbia.edu (G.M.) or or38@columbia.edu (O.H.) </help> </tool>