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changeset 7:edf43f311743 draft

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Deleted selected files
author david-hoover
date Wed, 12 Sep 2012 11:57:43 -0400
parents 2cef58c36b0f
children f60178b1a3dd
files gatk2_annotations.txt.sample gatk2_sorted_picard_index.loc.sample gatk2_wrapper.py tool_data_table_conf.xml.sample unified_genotyper.xml
diffstat 5 files changed, 0 insertions(+), 817 deletions(-) [+]
line wrap: on
line diff
--- a/gatk2_annotations.txt.sample	Wed Sep 12 11:41:34 2012 -0400
+++ /dev/null	Thu Jan 01 00:00:00 1970 +0000
@@ -1,30 +0,0 @@
-#unique_id	name	gatk_value	tools_valid_for
-AlleleBalance	AlleleBalance	AlleleBalance	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-AlleleBalanceBySample	AlleleBalanceBySample	AlleleBalanceBySample	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-BaseCounts	BaseCounts	BaseCounts	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-BaseQualityRankSumTest	BaseQualityRankSumTest	BaseQualityRankSumTest	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-ChromosomeCounts	ChromosomeCounts	ChromosomeCounts	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-DepthOfCoverage	DepthOfCoverage	DepthOfCoverage	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-DepthPerAlleleBySample	DepthPerAlleleBySample	DepthPerAlleleBySample	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-FisherStrand	FisherStrand	FisherStrand	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-GCContent	GCContent	GCContent	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-HaplotypeScore	HaplotypeScore	HaplotypeScore	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-HardyWeinberg	HardyWeinberg	HardyWeinberg	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-HomopolymerRun	HomopolymerRun	HomopolymerRun	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-InbreedingCoeff	InbreedingCoeff	InbreedingCoeff	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-IndelType	IndelType	IndelType	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-LowMQ	LowMQ	LowMQ	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-MVLikelihoodRatio	MVLikelihoodRatio	MVLikelihoodRatio	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-MappingQualityRankSumTest	MappingQualityRankSumTest	MappingQualityRankSumTest	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-MappingQualityZero	MappingQualityZero	MappingQualityZero	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-MappingQualityZeroBySample	MappingQualityZeroBySample	MappingQualityZeroBySample	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-MappingQualityZeroFraction	MappingQualityZeroFraction	MappingQualityZeroFraction	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-NBaseCount	NBaseCount	NBaseCount	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-QualByDepth	QualByDepth	QualByDepth	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-RMSMappingQuality	RMSMappingQuality	RMSMappingQuality	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-ReadDepthAndAllelicFractionBySample	ReadDepthAndAllelicFractionBySample	ReadDepthAndAllelicFractionBySample	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-ReadPosRankSumTest	ReadPosRankSumTest	ReadPosRankSumTest	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-SampleList	SampleList	SampleList	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-SnpEff	SnpEff	SnpEff	VariantAnnotator,VariantRecalibrator
-SpanningDeletions	SpanningDeletions	SpanningDeletions	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
-TechnologyComposition	TechnologyComposition	TechnologyComposition	UnifiedGenotyper,VariantAnnotator,VariantRecalibrator
--- a/gatk2_sorted_picard_index.loc.sample	Wed Sep 12 11:41:34 2012 -0400
+++ /dev/null	Thu Jan 01 00:00:00 1970 +0000
@@ -1,38 +0,0 @@
-#This is a sample file distributed with Galaxy that enables tools
-#to use a directory of Picard dict and associated files. You will need
-#to create these data files and then create a picard_index.loc file 
-#similar to this one (store it in this directory) that points to 
-#the directories in which those files are stored. The picard_index.loc 
-#file has this format (longer white space is the TAB character):
-#
-#<unique_build_id>	<dbkey>		<display_name>		<fasta_file_path>
-#
-#So, for example, if you had hg18 indexed and stored in 
-#/depot/data2/galaxy/srma/hg18/,
-#then the srma_index.loc entry would look like this:
-#
-#hg18	hg18	hg18 Pretty		/depot/data2/galaxy/picard/hg18/hg18.fa
-#
-#and your /depot/data2/galaxy/srma/hg18/ directory
-#would contain the following three files:
-#hg18.fa
-#hg18.dict
-#hg18.fa.fai
-#
-#The dictionary file for each reference (ex. hg18.dict) must be 
-#created via Picard (http://picard.sourceforge.net). Note that
-#the dict file does not have the .fa extension although the
-#path list in the loc file does include it.
-#
-dm3	dm3	dm3	/data/galaxy/ext-tool-data/picard/dm3.fa
-equCab2	equCab2	equCab2	/data/galaxy/ext-tool-data/picard/equCab2.fa
-hg17	hg17	hg17	/data/galaxy/ext-tool-data/picard/hg17.fa
-hg18	hg18	hg18	/data/galaxy/ext-tool-data/picard/hg18.fa
-hg19	hg19	hg19	/data/galaxy/ext-tool-data/picard/hg19.fa
-mm8	mm8	mm8	/data/galaxy/ext-tool-data/picard/mm8.fa
-mm9	mm9	mm9	/data/galaxy/ext-tool-data/picard/mm9.fa
-mm10	mm10	mm10	/data/galaxy/ext-tool-data/picard/mm10.fa
-rn4	rn4	rn4	/data/galaxy/ext-tool-data/picard/rn4.fa
-sacCer2	sacCer2	sacCer2	/data/galaxy/ext-tool-data/picard/sacCer2.fa
-sacCer3	sacCer3	sacCer3	/data/galaxy/ext-tool-data/picard/sacCer3.fa
-xenTro2	xenTro2	xenTro2	/data/galaxy/ext-tool-data/picard/xenTro2.fa
--- a/gatk2_wrapper.py	Wed Sep 12 11:41:34 2012 -0400
+++ /dev/null	Thu Jan 01 00:00:00 1970 +0000
@@ -1,126 +0,0 @@
-#!/usr/bin/env python
-#David Hoover, based on gatk by Dan Blankenberg
-
-"""
-A wrapper script for running the GenomeAnalysisTK.jar commands.
-"""
-
-import sys, optparse, os, tempfile, subprocess, shutil
-from binascii import unhexlify
-from string import Template
-
-GALAXY_EXT_TO_GATK_EXT = { 'gatk_interval':'intervals', 'bam_index':'bam.bai', 'gatk_dbsnp':'dbSNP', 'picard_interval_list':'interval_list' } #items not listed here will use the galaxy extension as-is
-GALAXY_EXT_TO_GATK_FILE_TYPE = GALAXY_EXT_TO_GATK_EXT #for now, these are the same, but could be different if needed
-DEFAULT_GATK_PREFIX = "gatk_file"
-CHUNK_SIZE = 2**20 #1mb
-
-
-def cleanup_before_exit( tmp_dir ):
-    if tmp_dir and os.path.exists( tmp_dir ):
-        shutil.rmtree( tmp_dir )
-
-def gatk_filename_from_galaxy( galaxy_filename, galaxy_ext, target_dir = None, prefix = None ):
-    suffix = GALAXY_EXT_TO_GATK_EXT.get( galaxy_ext, galaxy_ext )
-    if prefix is None:
-        prefix = DEFAULT_GATK_PREFIX
-    if target_dir is None:
-        target_dir = os.getcwd()
-    gatk_filename = os.path.join( target_dir, "%s.%s" % ( prefix, suffix ) )
-    os.symlink( galaxy_filename, gatk_filename )
-    return gatk_filename
-
-def gatk_filetype_argument_substitution( argument, galaxy_ext ):
-    return argument % dict( file_type = GALAXY_EXT_TO_GATK_FILE_TYPE.get( galaxy_ext, galaxy_ext ) )
-
-def open_file_from_option( filename, mode = 'rb' ):
-    if filename:
-        return open( filename, mode = mode )
-    return None
-
-def html_report_from_directory( html_out, dir ):
-    html_out.write( '<html>\n<head>\n<title>Galaxy - GATK Output</title>\n</head>\n<body>\n<p/>\n<ul>\n' )
-    for fname in sorted( os.listdir( dir ) ):
-        html_out.write(  '<li><a href="%s">%s</a></li>\n' % ( fname, fname ) )
-    html_out.write( '</ul>\n</body>\n</html>\n' )
-
-def index_bam_files( bam_filenames, tmp_dir ):
-    for bam_filename in bam_filenames:
-        bam_index_filename = "%s.bai" % bam_filename
-        if not os.path.exists( bam_index_filename ):
-            #need to index this bam file
-            stderr_name = tempfile.NamedTemporaryFile( prefix = "bam_index_stderr" ).name
-            command = 'samtools index %s %s' % ( bam_filename, bam_index_filename )
-            proc = subprocess.Popen( args=command, shell=True, stderr=open( stderr_name, 'wb' ) )
-            return_code = proc.wait()
-            if return_code:
-                for line in open( stderr_name ):
-                    print >> sys.stderr, line
-                os.unlink( stderr_name ) #clean up
-                cleanup_before_exit( tmp_dir )
-                raise Exception( "Error indexing BAM file" )
-            os.unlink( stderr_name ) #clean up
-
-def __main__():
-    #Parse Command Line
-    parser = optparse.OptionParser()
-    parser.add_option( '-p', '--pass_through', dest='pass_through_options', action='append', type="string", help='These options are passed through directly to GATK, without any modification.' )
-    parser.add_option( '-o', '--pass_through_options', dest='pass_through_options_encoded', action='append', type="string", help='These options are passed through directly to GATK, with decoding from binascii.unhexlify.' )
-    parser.add_option( '-d', '--dataset', dest='datasets', action='append', type="string", nargs=4, help='"-argument" "original_filename" "galaxy_filetype" "name_prefix"' )
-    parser.add_option( '', '--max_jvm_heap', dest='max_jvm_heap', action='store', type="string", default=None, help='If specified, the maximum java virtual machine heap size will be set to the provide value.' )
-    parser.add_option( '', '--max_jvm_heap_fraction', dest='max_jvm_heap_fraction', action='store', type="int", default=None, help='If specified, the maximum java virtual machine heap size will be set to the provide value as a fraction of total physical memory.' )
-    parser.add_option( '', '--stdout', dest='stdout', action='store', type="string", default=None, help='If specified, the output of stdout will be written to this file.' )
-    parser.add_option( '', '--stderr', dest='stderr', action='store', type="string", default=None, help='If specified, the output of stderr will be written to this file.' )
-    parser.add_option( '', '--html_report_from_directory', dest='html_report_from_directory', action='append', type="string", nargs=2, help='"Target HTML File" "Directory"')
-    (options, args) = parser.parse_args()
-    
-    tmp_dir = tempfile.mkdtemp( prefix='tmp-gatk-' )
-    if options.pass_through_options:
-        cmd = ' '.join( options.pass_through_options )
-    else:
-        cmd = ''
-    if options.pass_through_options_encoded:
-        cmd = '%s %s' % ( cmd, ' '.join( map( unhexlify, options.pass_through_options_encoded ) ) )
-    if options.max_jvm_heap is not None:
-        cmd = cmd.replace( 'java ', 'java -Xmx%s ' % ( options.max_jvm_heap ), 1 )
-    elif options.max_jvm_heap_fraction is not None:
-        cmd = cmd.replace( 'java ', 'java -XX:DefaultMaxRAMFraction=%s  -XX:+UseParallelGC ' % ( options.max_jvm_heap_fraction ), 1 )
-    bam_filenames = []
-    if options.datasets:
-        for ( dataset_arg, filename, galaxy_ext, prefix ) in options.datasets:
-            gatk_filename = gatk_filename_from_galaxy( filename, galaxy_ext, target_dir = tmp_dir, prefix = prefix )
-            if dataset_arg:
-                cmd = '%s %s "%s"' % ( cmd, gatk_filetype_argument_substitution( dataset_arg, galaxy_ext ), gatk_filename )
-            if galaxy_ext == "bam":
-                bam_filenames.append( gatk_filename )
-    index_bam_files( bam_filenames, tmp_dir )
-    #set up stdout and stderr output options
-    stdout = open_file_from_option( options.stdout, mode = 'wb' )
-    stderr = open_file_from_option( options.stderr, mode = 'wb' )
-    #if no stderr file is specified, we'll use our own
-    if stderr is None:
-        stderr = tempfile.NamedTemporaryFile( prefix="gatk-stderr-", dir=tmp_dir )
-    
-    proc = subprocess.Popen( args=cmd, stdout=stdout, stderr=stderr, shell=True, cwd=tmp_dir )
-    return_code = proc.wait()
-    
-    if return_code:
-        stderr_target = sys.stderr
-    else:
-        stderr_target = sys.stdout
-    stderr.flush()
-    stderr.seek(0)
-    while True:
-        chunk = stderr.read( CHUNK_SIZE )
-        if chunk:
-            stderr_target.write( chunk )
-        else:
-            break
-    stderr.close()
-    #generate html reports
-    if options.html_report_from_directory:
-        for ( html_filename, html_dir ) in options.html_report_from_directory:
-            html_report_from_directory( open( html_filename, 'wb' ), html_dir )
-    
-    cleanup_before_exit( tmp_dir )
-
-if __name__=="__main__": __main__()
--- a/tool_data_table_conf.xml.sample	Wed Sep 12 11:41:34 2012 -0400
+++ /dev/null	Thu Jan 01 00:00:00 1970 +0000
@@ -1,12 +0,0 @@
-<tables>
-    <!-- Location of Picard dict files valid for GATK -->
-    <table name="gatk2_picard_indexes" comment_char="#">
-        <columns>value, dbkey, name, path</columns>
-        <file path="tool-data/gatk2_sorted_picard_index.loc" />
-    </table>
-    <!-- Available of GATK references -->
-    <table name="gatk2_annotations" comment_char="#">
-        <columns>value, name, gatk_value, tools_valid_for</columns>
-        <file path="tool-data/gatk2_annotations.txt" />
-    </table>
-</tables>
--- a/unified_genotyper.xml	Wed Sep 12 11:41:34 2012 -0400
+++ /dev/null	Thu Jan 01 00:00:00 1970 +0000
@@ -1,611 +0,0 @@
-<tool id="gatk2_unified_genotyper" name="Unified Genotyper" version="0.0.1">
-  <description>SNP and indel caller</description>
-  <requirements>
-      <requirement type="package" version="2.1">gatk2</requirement>
-      <requirement type="package" version="0.1.18">samtools</requirement>
-  </requirements>
-  <command interpreter="python">gatk2_wrapper.py
-   --max_jvm_heap_fraction "1"
-   --stdout "${output_log}"
-   #for $i, $input_bam in enumerate( $reference_source.input_bams ):
-       -d "-I" "${input_bam.input_bam}" "${input_bam.input_bam.ext}" "gatk_input_${i}"
-       #if str( $input_bam.input_bam.metadata.bam_index ) != "None":
-           -d "" "${input_bam.input_bam.metadata.bam_index}" "bam_index" "gatk_input_${i}" ##hardcode galaxy ext type as bam_index
-       #end if
-   #end for
-   -p 'java 
-    -jar "GenomeAnalysisTK.jar"
-    -T "UnifiedGenotyper"
-    --num_threads 4 ##hard coded, for now
-    --out "${output_vcf}"
-    --metrics_file "${output_metrics}"
-    -et "NO_ET" -K "gatk2_key_file" ##ET no phone home
-    ##-log "${output_log}" ##don't use this to log to file, instead directly capture stdout
-    #if $reference_source.reference_source_selector != "history":
-        -R "${reference_source.ref_file.fields.path}"
-    #end if
-    --genotype_likelihoods_model "${genotype_likelihoods_model}"
-    --standard_min_confidence_threshold_for_calling "${standard_min_confidence_threshold_for_calling}"
-    --standard_min_confidence_threshold_for_emitting "${standard_min_confidence_threshold_for_emitting}"
-   '
-    #set $rod_binding_names = dict()
-    #for $rod_binding in $rod_bind:
-        #if str( $rod_binding.rod_bind_type.rod_bind_type_selector ) == 'custom':
-            #set $rod_bind_name = $rod_binding.rod_bind_type.custom_rod_name
-        #else
-            #set $rod_bind_name = $rod_binding.rod_bind_type.rod_bind_type_selector
-        #end if
-        #set $rod_binding_names[$rod_bind_name] = $rod_binding_names.get( $rod_bind_name, -1 ) + 1
-        -d "--dbsnp:${rod_bind_name},%(file_type)s" "${rod_binding.rod_bind_type.input_rod}" "${rod_binding.rod_bind_type.input_rod.ext}" "input_${rod_bind_name}_${rod_binding_names[$rod_bind_name]}"
-    #end for
-   
-    ##start standard gatk options
-    #if $gatk_param_type.gatk_param_type_selector == "advanced":
-        #for $pedigree in $gatk_param_type.pedigree:
-            -p '--pedigree "${pedigree.pedigree_file}"'
-        #end for
-        #for $pedigree_string in $gatk_param_type.pedigree_string_repeat:
-            -p '--pedigreeString "${pedigree_string.pedigree_string}"'
-        #end for
-        -p '--pedigreeValidationType "${gatk_param_type.pedigree_validation_type}"'
-        #for $read_filter in $gatk_param_type.read_filter:
-            -p '--read_filter "${read_filter.read_filter_type.read_filter_type_selector}"
-            ###raise Exception( str( dir( $read_filter ) ) )
-            #for $name, $param in $read_filter.read_filter_type.iteritems():
-                #if $name not in [ "__current_case__", "read_filter_type_selector" ]:
-                    #if hasattr( $param.input, 'truevalue' ):
-                        ${param}
-                    #else:
-                        --${name} "${param}"
-                    #end if
-                #end if
-            #end for
-            '
-        #end for
-        #for $interval_count, $input_intervals in enumerate( $gatk_param_type.input_interval_repeat ):
-            -d "--intervals" "${input_intervals.input_intervals}" "${input_intervals.input_intervals.ext}" "input_intervals_${interval_count}"
-        #end for
-        
-        #for $interval_count, $input_intervals in enumerate( $gatk_param_type.input_exclude_interval_repeat ):
-            -d "--excludeIntervals" "${input_intervals.input_exclude_intervals}" "${input_intervals.input_exclude_intervals.ext}" "input_exlude_intervals_${interval_count}"
-        #end for
-
-        -p '--interval_set_rule "${gatk_param_type.interval_set_rule}"'
-        
-        -p '--downsampling_type "${gatk_param_type.downsampling_type.downsampling_type_selector}"'
-        #if str( $gatk_param_type.downsampling_type.downsampling_type_selector ) != "NONE":
-            -p '--${gatk_param_type.downsampling_type.downsample_to_type.downsample_to_type_selector} "${gatk_param_type.downsampling_type.downsample_to_type.downsample_to_value}"'
-        #end if
-        -p '
-        --baq "${gatk_param_type.baq}"
-        --baqGapOpenPenalty "${gatk_param_type.baq_gap_open_penalty}"
-        ${gatk_param_type.use_original_qualities}
-        --defaultBaseQualities "${gatk_param_type.default_base_qualities}"
-        --validation_strictness "${gatk_param_type.validation_strictness}"
-        --interval_merging "${gatk_param_type.interval_merging}"
-        ${gatk_param_type.disable_experimental_low_memory_sharding}
-        ${gatk_param_type.non_deterministic_random_seed}
-        '
-        #for $rg_black_list_count, $rg_black_list in enumerate( $gatk_param_type.read_group_black_list_repeat ):
-            #if $rg_black_list.read_group_black_list_type.read_group_black_list_type_selector == "file":
-                -d "--read_group_black_list" "${rg_black_list.read_group_black_list_type.read_group_black_list}" "txt" "input_read_group_black_list_${rg_black_list_count}"
-            #else
-                -p '--read_group_black_list "${rg_black_list.read_group_black_list_type.read_group_black_list}"'
-            #end if
-        #end for
-    #end if
-    
-    #if $reference_source.reference_source_selector == "history":
-        -d "-R" "${reference_source.ref_file}" "${reference_source.ref_file.ext}" "gatk_input"
-    #end if
-    ##end standard gatk options
-    ##start analysis specific options
-    #if $analysis_param_type.analysis_param_type_selector == "advanced":
-        -p '
-        --p_nonref_model "${analysis_param_type.p_nonref_model}"
-        --heterozygosity "${analysis_param_type.heterozygosity}"
-        --pcr_error_rate "${analysis_param_type.pcr_error_rate}"
-        --genotyping_mode "${analysis_param_type.genotyping_mode_type.genotyping_mode}"
-        #if str( $analysis_param_type.genotyping_mode_type.genotyping_mode ) == 'GENOTYPE_GIVEN_ALLELES':
-            --alleles "${analysis_param_type.genotyping_mode_type.input_alleles_rod}"
-        #end if
-        --output_mode "${analysis_param_type.output_mode}"
-        ${analysis_param_type.compute_SLOD}
-        --min_base_quality_score "${analysis_param_type.min_base_quality_score}"
-        --max_deletion_fraction "${analysis_param_type.max_deletion_fraction}"
-        --max_alternate_alleles "${analysis_param_type.max_alternate_alleles}"
-        --min_indel_count_for_genotyping "${analysis_param_type.min_indel_count_for_genotyping}"
-        --indel_heterozygosity "${analysis_param_type.indel_heterozygosity}"
-        --indelGapContinuationPenalty "${analysis_param_type.indelGapContinuationPenalty}"
-        --indelGapOpenPenalty "${analysis_param_type.indelGapOpenPenalty}"
-        --indelHaplotypeSize "${analysis_param_type.indelHaplotypeSize}"
-        ${analysis_param_type.doContextDependentGapPenalties}
-        #if str( $analysis_param_type.annotation ) != "None":
-            #for $annotation in str( $analysis_param_type.annotation.fields.gatk_value ).split( ','):
-                --annotation "${annotation}"
-            #end for
-        #end if
-        #for $additional_annotation in $analysis_param_type.additional_annotations:
-            --annotation "${additional_annotation.additional_annotation_name}"
-        #end for
-        #if str( $analysis_param_type.group ) != "None":
-            #for $group in str( $analysis_param_type.group ).split( ','):
-                --group "${group}"
-            #end for
-        #end if
-        #if str( $analysis_param_type.exclude_annotations ) != "None":
-            #for $annotation in str( $analysis_param_type.exclude_annotations.fields.gatk_value ).split( ','):
-                --excludeAnnotation "${annotation}"
-            #end for
-        #end if
-        ${analysis_param_type.multiallelic}
-        '
-##        #if str( $analysis_param_type.snpEff_rod_bind_type.snpEff_rod_bind_type_selector ) == 'set_snpEff':
-##            -p '--annotation "SnpEff"'
-##            -d "--snpEffFile:${analysis_param_type.snpEff_rod_bind_type.snpEff_rod_name},%(file_type)s" "${analysis_param_type.snpEff_rod_bind_type.snpEff_input_rod}" "${analysis_param_type.snpEff_rod_bind_type.snpEff_input_rod.ext}" "input_snpEff_${analysis_param_type.snpEff_rod_bind_type.snpEff_rod_name}"
-##        #else:
-##            -p '--excludeAnnotation "SnpEff"'
-##        #end if
-    #end if
-  </command>
-  <inputs>
-    <conditional name="reference_source">
-      <param name="reference_source_selector" type="select" label="Choose the source for the reference list">
-        <option value="cached">Locally cached</option>
-        <option value="history">History</option>
-      </param>
-      <when value="cached">
-        <repeat name="input_bams" title="BAM file" min="1" help="-I,--input_file &amp;lt;input_file&amp;gt;">
-            <param name="input_bam" type="data" format="bam" label="BAM file">
-              <validator type="unspecified_build" />
-              <validator type="dataset_metadata_in_data_table" table_name="gatk2_picard_indexes" metadata_name="dbkey" metadata_column="dbkey" message="Sequences are not currently available for the specified build." /> <!-- fixme!!! this needs to be a select -->
-            </param>
-        </repeat>
-        <param name="ref_file" type="select" label="Using reference genome" help="-R,--reference_sequence &amp;lt;reference_sequence&amp;gt;">
-          <options from_data_table="gatk2_picard_indexes">
-            <!-- <filter type="data_meta" key="dbkey" ref="input_bam" column="dbkey"/> does not yet work in a repeat...--> 
-          </options>
-          <validator type="no_options" message="A built-in reference genome is not available for the build associated with the selected input file"/>
-        </param>
-      </when>
-      <when value="history"> <!-- FIX ME!!!! -->
-        <repeat name="input_bams" title="BAM file" min="1" help="-I,--input_file &amp;lt;input_file&amp;gt;">
-            <param name="input_bam" type="data" format="bam" label="BAM file" >
-            </param>
-        </repeat>
-        <param name="ref_file" type="data" format="fasta" label="Using reference file" help="-R,--reference_sequence &amp;lt;reference_sequence&amp;gt;" />
-      </when>
-    </conditional>
-    
-    <repeat name="rod_bind" title="Binding for reference-ordered data" help="-D,--dbsnp &amp;lt;dbsnp&amp;gt;">
-        <conditional name="rod_bind_type">
-          <param name="rod_bind_type_selector" type="select" label="Binding Type">
-            <option value="dbsnp" selected="True">dbSNP</option>
-            <option value="snps">SNPs</option>
-            <option value="indels">INDELs</option>
-            <option value="custom">Custom</option>
-          </param>
-          <when value="dbsnp">
-              <param name="input_rod" type="data" format="vcf" label="ROD file" />
-          </when>
-          <when value="snps">
-              <param name="input_rod" type="data" format="vcf" label="ROD file" />
-          </when>
-          <when value="indels">
-              <param name="input_rod" type="data" format="vcf" label="ROD file" />
-          </when>
-          <when value="custom">
-              <param name="custom_rod_name" type="text" value="Unknown" label="ROD Name"/>
-              <param name="input_rod" type="data" format="vcf" label="ROD file" />
-          </when>
-        </conditional>
-    </repeat>
-    
-    <param name="genotype_likelihoods_model" type="select" label="Genotype likelihoods calculation model to employ" help="-glm,--genotype_likelihoods_model &amp;lt;genotype_likelihoods_model&amp;gt;">
-      <option value="BOTH" selected="True">BOTH</option>
-      <option value="SNP">SNP</option>
-      <option value="INDEL">INDEL</option>
-    </param>
-    
-    <param name="standard_min_confidence_threshold_for_calling" type="float" value="30.0" label="The minimum phred-scaled confidence threshold at which variants not at 'trigger' track sites should be called" help="-stand_call_conf,--standard_min_confidence_threshold_for_calling &amp;lt;standard_min_confidence_threshold_for_calling&amp;gt;" />
-    <param name="standard_min_confidence_threshold_for_emitting" type="float" value="30.0" label="The minimum phred-scaled confidence threshold at which variants not at 'trigger' track sites should be emitted (and filtered if less than the calling threshold)" help="-stand_emit_conf,--standard_min_confidence_threshold_for_emitting &amp;lt;standard_min_confidence_threshold_for_emitting&amp;gt;" />
-
-    
-    <conditional name="gatk_param_type">
-      <param name="gatk_param_type_selector" type="select" label="Basic or Advanced GATK options">
-        <option value="basic" selected="True">Basic</option>
-        <option value="advanced">Advanced</option>
-      </param>
-      <when value="basic">
-        <!-- Do nothing here -->
-      </when>
-      <when value="advanced">
-        <repeat name="pedigree" title="Pedigree file" help="-ped,--pedigree &amp;lt;pedigree&amp;gt;">
-            <param name="pedigree_file" type="data" format="txt" label="Pedigree files for samples"/>
-        </repeat>
-        <repeat name="pedigree_string_repeat" title="Pedigree string" help="-pedString,--pedigreeString &amp;lt;pedigreeString&amp;gt;">
-            <param name="pedigree_string" type="text" value="" label="Pedigree string for samples"/>
-        </repeat>
-        <param name="pedigree_validation_type" type="select" label="How strict should we be in validating the pedigree information" help="-pedValidationType,--pedigreeValidationType &amp;lt;pedigreeValidationType&amp;gt;">
-          <option value="STRICT" selected="True">STRICT</option>
-          <option value="SILENT">SILENT</option>
-        </param>
-        <repeat name="read_filter" title="Read Filter" help="-rf,--read_filter &amp;lt;read_filter&amp;gt;">
-            <conditional name="read_filter_type">
-              <param name="read_filter_type_selector" type="select" label="Read Filter Type">
-                <option value="BadCigar">BadCigar</option>
-                <option value="BadMate">BadMate</option>
-                <option value="DuplicateRead">DuplicateRead</option>
-                <option value="FailsVendorQualityCheck">FailsVendorQualityCheck</option>
-                <option value="MalformedRead">MalformedRead</option>
-                <option value="MappingQuality">MappingQuality</option>
-                <option value="MappingQualityUnavailable">MappingQualityUnavailable</option>
-                <option value="MappingQualityZero">MappingQualityZero</option>
-                <option value="MateSameStrand">MateSameStrand</option>
-                <option value="MaxInsertSize">MaxInsertSize</option>
-                <option value="MaxReadLength" selected="True">MaxReadLength</option>
-                <option value="MissingReadGroup">MissingReadGroup</option>
-                <option value="NoOriginalQualityScores">NoOriginalQualityScores</option>
-                <option value="NotPrimaryAlignment">NotPrimaryAlignment</option>
-                <option value="Platform454">Platform454</option>
-                <option value="Platform">Platform</option>
-                <option value="PlatformUnit">PlatformUnit</option>
-                <option value="ReadGroupBlackList">ReadGroupBlackList</option>
-                <option value="ReadName">ReadName</option>
-                <option value="ReadStrand">ReadStrand</option>
-                <option value="ReassignMappingQuality">ReassignMappingQuality</option>
-                <option value="Sample">Sample</option>
-                <option value="SingleReadGroup">SingleReadGroup</option>
-                <option value="UnmappedRead">UnmappedRead</option>
-              </param>
-              <when value="BadCigar">
-                  <!-- no extra options -->
-              </when>
-              <when value="BadMate">
-                  <!-- no extra options -->
-              </when>
-              <when value="DuplicateRead">
-                  <!-- no extra options -->
-              </when>
-              <when value="FailsVendorQualityCheck">
-                  <!-- no extra options -->
-              </when>
-              <when value="MalformedRead">
-                  <!-- no extra options -->
-              </when>
-              <when value="MappingQuality">
-                  <param name="min_mapping_quality_score" type="integer" value="10" label="Minimum read mapping quality required to consider a read for calling"/>
-              </when>
-              <when value="MappingQualityUnavailable">
-                  <!-- no extra options -->
-              </when>
-              <when value="MappingQualityZero">
-                  <!-- no extra options -->
-              </when>
-              <when value="MateSameStrand">
-                  <!-- no extra options -->
-              </when>
-              <when value="MaxInsertSize">
-                  <param name="maxInsertSize" type="integer" value="1000000" label="Discard reads with insert size greater than the specified value"/>
-              </when>
-              <when value="MaxReadLength">
-                  <param name="maxReadLength" type="integer" value="76" label="Max Read Length"/>
-              </when>
-              <when value="MissingReadGroup">
-                  <!-- no extra options -->
-              </when>
-              <when value="NoOriginalQualityScores">
-                  <!-- no extra options -->
-              </when>
-              <when value="NotPrimaryAlignment">
-                  <!-- no extra options -->
-              </when>
-              <when value="Platform454">
-                  <!-- no extra options -->
-              </when>
-              <when value="Platform">
-                  <param name="PLFilterName" type="text" value="" label="Discard reads with RG:PL attribute containing this string"/>
-              </when>
-              <when value="PlatformUnit">
-                  <!-- no extra options -->
-              </when>
-              <when value="ReadGroupBlackList">
-                  <!-- no extra options -->
-              </when>
-              <when value="ReadName">
-                  <param name="readName" type="text" value="" label="Filter out all reads except those with this read name"/>
-              </when>
-              <when value="ReadStrand">
-                  <param name="filterPositive" type="boolean" truevalue="--filterPositive" falsevalue="" label="Discard reads on the forward strand"/>
-              </when>
-              <when value="ReassignMappingQuality">
-                  <param name="default_mapping_quality" type="integer" value="60" label="Default read mapping quality to assign to all reads"/>
-              </when>
-              <when value="Sample">
-                  <param name="sample_to_keep" type="text" value="" label="The name of the sample(s) to keep, filtering out all others"/>
-              </when>
-              <when value="SingleReadGroup">
-                  <param name="read_group_to_keep" type="integer" value="76" label="The name of the read group to keep, filtering out all others"/>
-              </when>
-              <when value="UnmappedRead">
-                  <!-- no extra options -->
-              </when>
-            </conditional>
-        </repeat>
-        <repeat name="input_interval_repeat" title="Operate on Genomic intervals" help="-L,--intervals &amp;lt;intervals&amp;gt;">
-          <param name="input_intervals" type="data" format="bed,gatk_interval,picard_interval_list,vcf" label="Genomic intervals" />
-        </repeat>
-        <repeat name="input_exclude_interval_repeat" title="Exclude Genomic intervals" help="-XL,--excludeIntervals &amp;lt;excludeIntervals&amp;gt;">
-          <param name="input_exclude_intervals" type="data" format="bed,gatk_interval,picard_interval_list,vcf" label="Genomic intervals" />
-        </repeat>
-        
-        <param name="interval_set_rule" type="select" label="Interval set rule" help="-isr,--interval_set_rule &amp;lt;interval_set_rule&amp;gt;">
-          <option value="UNION" selected="True">UNION</option>
-          <option value="INTERSECTION">INTERSECTION</option>
-        </param>
-        
-        <conditional name="downsampling_type">
-          <param name="downsampling_type_selector" type="select" label="Type of reads downsampling to employ at a given locus" help="-dt,--downsampling_type &amp;lt;downsampling_type&amp;gt;">
-            <option value="NONE" selected="True">NONE</option>
-            <option value="ALL_READS">ALL_READS</option>
-            <option value="BY_SAMPLE">BY_SAMPLE</option>
-          </param>
-          <when value="NONE">
-              <!-- no more options here -->
-          </when>
-          <when value="ALL_READS">
-              <conditional name="downsample_to_type">
-                  <param name="downsample_to_type_selector" type="select" label="Downsample method">
-                      <option value="downsample_to_fraction" selected="True">Downsample by Fraction</option>
-                      <option value="downsample_to_coverage">Downsample by Coverage</option>
-                  </param>
-                  <when value="downsample_to_fraction">
-                      <param name="downsample_to_value" type="float" label="Fraction [0.0-1.0] of reads to downsample to" value="1" min="0" max="1" help="-dfrac,--downsample_to_fraction &amp;lt;downsample_to_fraction&amp;gt;"/>
-                  </when>
-                  <when value="downsample_to_coverage">
-                      <param name="downsample_to_value" type="integer" label="Coverage to downsample to at any given locus" value="0" help="-dcov,--downsample_to_coverage &amp;lt;downsample_to_coverage&amp;gt;"/>
-                  </when>
-              </conditional>
-          </when>
-          <when value="BY_SAMPLE">
-              <conditional name="downsample_to_type">
-                  <param name="downsample_to_type_selector" type="select" label="Downsample method">
-                      <option value="downsample_to_fraction" selected="True">Downsample by Fraction</option>
-                      <option value="downsample_to_coverage">Downsample by Coverage</option>
-                  </param>
-                  <when value="downsample_to_fraction">
-                      <param name="downsample_to_value" type="float" label="Fraction [0.0-1.0] of reads to downsample to" value="1" min="0" max="1" help="-dfrac,--downsample_to_fraction &amp;lt;downsample_to_fraction&amp;gt;"/>
-                  </when>
-                  <when value="downsample_to_coverage">
-                      <param name="downsample_to_value" type="integer" label="Coverage to downsample to at any given locus" value="0" help="-dcov,--downsample_to_coverage &amp;lt;downsample_to_coverage&amp;gt;"/>
-                  </when>
-              </conditional>
-          </when>
-        </conditional>
-        <param name="baq" type="select" label="Type of BAQ calculation to apply in the engine" help="-baq,--baq &amp;lt;baq&amp;gt;">
-          <option value="OFF" selected="True">OFF</option>
-          <option value="CALCULATE_AS_NECESSARY">CALCULATE_AS_NECESSARY</option>
-          <option value="RECALCULATE">RECALCULATE</option>
-        </param>
-        <param name="baq_gap_open_penalty" type="float" label="BAQ gap open penalty (Phred Scaled)" value="40" help="Default value is 40. 30 is perhaps better for whole genome call sets. -baqGOP,--baqGapOpenPenalty &amp;lt;baqGapOpenPenalty&amp;gt;" />
-        <param name="use_original_qualities" type="boolean" truevalue="--useOriginalQualities" falsevalue="" label="Use the original base quality scores from the OQ tag" help="-OQ,--useOriginalQualities" />
-        <param name="default_base_qualities" type="integer" label="Value to be used for all base quality scores, when some are missing" value="-1" help="-DBQ,--defaultBaseQualities &amp;lt;defaultBaseQualities&amp;gt;"/>
-        <param name="validation_strictness" type="select" label="How strict should we be with validation" help="-S,--validation_strictness &amp;lt;validation_strictness&amp;gt;">
-          <option value="STRICT" selected="True">STRICT</option>
-          <option value="LENIENT">LENIENT</option>
-          <option value="SILENT">SILENT</option>
-          <!-- <option value="DEFAULT_STRINGENCY">DEFAULT_STRINGENCY</option> listed in docs, but not valid value...-->
-        </param>
-        <param name="interval_merging" type="select" label="Interval merging rule" help="-im,--interval_merging &amp;lt;interval_merging&amp;gt;">
-          <option value="ALL" selected="True">ALL</option>
-          <option value="OVERLAPPING_ONLY">OVERLAPPING_ONLY</option>
-        </param>
-        
-        <repeat name="read_group_black_list_repeat" title="Read group black list" help="-rgbl,--read_group_black_list &amp;lt;read_group_black_list&amp;gt;">
-          <conditional name="read_group_black_list_type">
-            <param name="read_group_black_list_type_selector" type="select" label="Type of reads read group black list">
-              <option value="file" selected="True">Filters in file</option>
-              <option value="text">Specify filters as a string</option>
-            </param>
-            <when value="file">
-              <param name="read_group_black_list" type="data" format="txt" label="Read group black list file" />
-            </when>
-            <when value="text">
-              <param name="read_group_black_list" type="text" value="tag:string" label="Read group black list tag:string" />
-            </when>
-          </conditional>
-        </repeat>
-        
-        <param name="disable_experimental_low_memory_sharding" type="boolean" truevalue="--disable_experimental_low_memory_sharding" falsevalue="" label="Disable experimental low-memory sharding functionality." checked="False" help="--disable_experimental_low_memory_sharding"/>
-        <param name="non_deterministic_random_seed" type="boolean" truevalue="--nonDeterministicRandomSeed" falsevalue="" label="Makes the GATK behave non deterministically, that is, the random numbers generated will be different in every run" checked="False"  help="-ndrs,--nonDeterministicRandomSeed"/>
-        
-      </when>
-    </conditional>
-    
-    <conditional name="analysis_param_type">
-      <param name="analysis_param_type_selector" type="select" label="Basic or Advanced Analysis options">
-        <option value="basic" selected="True">Basic</option>
-        <option value="advanced">Advanced</option>
-      </param>
-      <when value="basic">
-        <!-- Do nothing here -->
-      </when>
-      <when value="advanced">
-        <param name="p_nonref_model" type="select" label="Non-reference probability calculation model to employ" help="-pnrm,--p_nonref_model &amp;lt;p_nonref_model&amp;gt;">
-          <option value="EXACT" selected="True">EXACT</option>
-          <option value="GRID_SEARCH">GRID_SEARCH</option>
-        </param>
-        <param name="heterozygosity" type="float" value="1e-3" label="Heterozygosity value used to compute prior likelihoods for any locus" help="-hets,--heterozygosity &amp;lt;heterozygosity&amp;gt;" />
-        <param name="pcr_error_rate" type="float" value="1e-4" label="The PCR error rate to be used for computing fragment-based likelihoods" help="-pcr_error,--pcr_error_rate &amp;lt;pcr_error_rate&amp;gt;" />
-        <conditional name="genotyping_mode_type">
-          <param name="genotyping_mode" type="select" label="How to determine the alternate allele to use for genotyping" help="-gt_mode,--genotyping_mode &amp;lt;genotyping_mode&amp;gt;">
-            <option value="DISCOVERY" selected="True">DISCOVERY</option>
-            <option value="GENOTYPE_GIVEN_ALLELES">GENOTYPE_GIVEN_ALLELES</option>
-          </param>
-          <when value="DISCOVERY">
-            <!-- Do nothing here -->
-          </when>
-          <when value="GENOTYPE_GIVEN_ALLELES">
-            <param name="input_alleles_rod" type="data" format="vcf" label="Alleles ROD file" help="-alleles,--alleles &amp;lt;alleles&amp;gt;" />
-          </when>
-        </conditional>
-        <param name="output_mode" type="select" label="Should we output confident genotypes (i.e. including ref calls) or just the variants?" help="-out_mode,--output_mode &amp;lt;output_mode&amp;gt;">
-          <option value="EMIT_VARIANTS_ONLY" selected="True">EMIT_VARIANTS_ONLY</option>
-          <option value="EMIT_ALL_CONFIDENT_SITES">EMIT_ALL_CONFIDENT_SITES</option>
-          <option value="EMIT_ALL_SITES">EMIT_ALL_SITES</option>
-        </param>
-        <param name="compute_SLOD" type="boolean" truevalue="--computeSLOD" falsevalue="" label="Compute the SLOD" help="--computeSLOD" />
-        <param name="min_base_quality_score" type="integer" value="17" label="Minimum base quality required to consider a base for calling" help="-mbq,--min_base_quality_score &amp;lt;min_base_quality_score&amp;gt;" />
-        <param name="max_deletion_fraction" type="float" value="0.05" label="Maximum fraction of reads with deletions spanning this locus for it to be callable" help="to disable, set to &lt; 0 or &gt; 1 (-deletions,--max_deletion_fraction &amp;lt;max_deletion_fraction&amp;gt;)" />
-        <param name="max_alternate_alleles" type="integer" value="5" label="Maximum number of alternate alleles to genotype" help="-maxAlleles,--max_alternate_alleles &amp;lt;max_alternate_alleles&amp;gt;" />
-        <param name="min_indel_count_for_genotyping" type="integer" value="5" label="Minimum number of consensus indels required to trigger genotyping run" help="-minIndelCnt,--min_indel_count_for_genotyping &amp;lt;min_indel_count_for_genotyping&amp;gt;" />
-        <param name="indel_heterozygosity" type="float" value="0.000125" label="Heterozygosity for indel calling" help="1.0/8000==0.000125 (-indelHeterozygosity,--indel_heterozygosity &amp;lt;indel_heterozygosity&amp;gt;)"/>
-        <param name="indelGapContinuationPenalty" type="float" value="10.0" label="Indel gap continuation penalty" help="--indelGapContinuationPenalty" />
-        <param name="indelGapOpenPenalty" type="float" value="45.0" label="Indel gap open penalty" help="--indelGapOpenPenalty" />
-        <param name="indelHaplotypeSize" type="integer" value="80" label="Indel haplotype size" help="--indelHaplotypeSize" />
-        <param name="doContextDependentGapPenalties" type="boolean" truevalue="--doContextDependentGapPenalties" falsevalue="" label="Vary gap penalties by context" help="--doContextDependentGapPenalties" />
-        <param name="annotation" type="select" multiple="True" display="checkboxes" label="Annotation Types" help="-A,--annotation &amp;lt;annotation&amp;gt;">
-          <!-- load the available annotations from an external configuration file, since additional ones can be added to local installs -->
-          <options from_data_table="gatk_annotations">
-            <filter type="multiple_splitter" column="tools_valid_for" separator=","/>
-            <filter type="static_value" value="UnifiedGenotyper" column="tools_valid_for"/>
-          </options>
-        </param>
-        <repeat name="additional_annotations" title="Additional annotation" help="-A,--annotation &amp;lt;annotation&amp;gt;">
-          <param name="additional_annotation_name" type="text" value="" label="Annotation name" />
-        </repeat>
-<!--
-        <conditional name="snpEff_rod_bind_type">
-          <param name="snpEff_rod_bind_type_selector" type="select" label="Provide a snpEff reference-ordered data file">
-            <option value="set_snpEff">Set snpEff</option>
-            <option value="exclude_snpEff" selected="True">Don't set snpEff</option>
-          </param>
-          <when value="exclude_snpEff">
-          </when>
-          <when value="set_snpEff">
-            <param name="snpEff_input_rod" type="data" format="vcf" label="ROD file" />
-            <param name="snpEff_rod_name" type="hidden" value="snpEff" label="ROD Name"/>
-          </when>
-        </conditional>
--->
-        <param name="group" type="select" multiple="True" display="checkboxes" label="Annotation Interfaces/Groups" help="-G,--group &amp;lt;group&amp;gt;">
-            <option value="RodRequiringAnnotation">RodRequiringAnnotation</option>
-            <option value="Standard">Standard</option>
-            <option value="Experimental">Experimental</option>
-            <option value="WorkInProgress">WorkInProgress</option>
-            <option value="RankSumTest">RankSumTest</option>
-            <!-- <option value="none">none</option> -->
-        </param>
-    <!--     <param name="family_string" type="text" value="" label="Family String"/> -->
-        <param name="exclude_annotations" type="select" multiple="True" display="checkboxes" label="Annotations to exclude" help="-XA,--excludeAnnotation &amp;lt;excludeAnnotation&amp;gt;" >
-          <!-- load the available annotations from an external configuration file, since additional ones can be added to local installs -->
-          <options from_data_table="gatk_annotations">
-            <filter type="multiple_splitter" column="tools_valid_for" separator=","/>
-            <filter type="static_value" value="UnifiedGenotyper" column="tools_valid_for"/>
-          </options>
-        </param>
-        <param name="multiallelic" type="boolean" truevalue="--multiallelic" falsevalue="" label="Allow the discovery of multiple alleles (SNPs only)" help="--multiallelic" />
-      </when>
-    </conditional>
-  </inputs>
-  <outputs>
-    <data format="vcf" name="output_vcf" label="${tool.name} on ${on_string} (VCF)" />
-    <data format="txt" name="output_metrics" label="${tool.name} on ${on_string} (metrics)" />
-    <data format="txt" name="output_log" label="${tool.name} on ${on_string} (log)" />
-  </outputs>
-  <trackster_conf/>
-  <tests>
-      <test>
-          <param name="reference_source_selector" value="history" />
-          <param name="ref_file" value="phiX.fasta" ftype="fasta" />
-          <param name="input_bam" value="gatk/gatk_table_recalibration/gatk_table_recalibration_out_1.bam" ftype="bam" />
-          <param name="rod_bind_type_selector" value="dbsnp" />
-          <param name="input_rod" value="gatk/fake_phiX_variant_locations.vcf" ftype="vcf" />
-          <param name="standard_min_confidence_threshold_for_calling" value="0" />
-          <param name="standard_min_confidence_threshold_for_emitting" value="4" />
-          <param name="gatk_param_type_selector" value="basic" />
-          <param name="analysis_param_type_selector" value="advanced" />
-          <param name="genotype_likelihoods_model" value="BOTH" />
-          <param name="p_nonref_model" value="EXACT" />
-          <param name="heterozygosity" value="0.001" />
-          <param name="pcr_error_rate" value="0.0001" />
-          <param name="genotyping_mode" value="DISCOVERY" />
-          <param name="output_mode" value="EMIT_ALL_CONFIDENT_SITES" />
-          <param name="compute_SLOD" />
-          <param name="min_base_quality_score" value="17" />
-          <param name="max_deletion_fraction" value="-1" />
-          <param name="min_indel_count_for_genotyping" value="2" />
-          <param name="indel_heterozygosity" value="0.000125" />
-          <param name="indelGapContinuationPenalty" value="10" />
-          <param name="indelGapOpenPenalty" value="3" />
-          <param name="indelHaplotypeSize" value="80" />
-          <param name="doContextDependentGapPenalties" />
-          <!-- <param name="annotation" value="" />
-          <param name="group" value="" /> -->
-          <output name="output_vcf" file="gatk/gatk_unified_genotyper/gatk_unified_genotyper_out_1.vcf" lines_diff="4" /> 
-          <output name="output_metrics" file="gatk/gatk_unified_genotyper/gatk_unified_genotyper_out_1.metrics" /> 
-          <output name="output_log" file="gatk/gatk_unified_genotyper/gatk_unified_genotyper_out_1.log.contains" compare="contains" />
-      </test>
-  </tests>
-  <help>
-**What it does**
-
-A variant caller which unifies the approaches of several disparate callers.  Works for single-sample and multi-sample data.  The user can choose from several different incorporated calculation models.
-
-For more information on the GATK Unified Genotyper, see this `tool specific page &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Unified_genotyper&gt;`_.
-
-To learn about best practices for variant detection using GATK, see this `overview &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Best_Practice_Variant_Detection_with_the_GATK_v3&gt;`_.
-
-If you encounter errors, please view the `GATK FAQ &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Frequently_Asked_Questions&gt;`_.
-
-------
-
-**Inputs**
-
-GenomeAnalysisTK: UnifiedGenotyper accepts an aligned BAM input file.
-
-
-**Outputs**
-
-The output is in VCF format.
-
-
-Go `here &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Input_files_for_the_GATK&gt;`_ for details on GATK file formats.
-
--------
-
-**Settings**::
-
- genotype_likelihoods_model                        Genotype likelihoods calculation model to employ -- BOTH is the default option, while INDEL is also available for calling indels and SNP is available for calling SNPs only (SNP|INDEL|BOTH)
- p_nonref_model                                    Non-reference probability calculation model to employ -- EXACT is the default option, while GRID_SEARCH is also available. (EXACT|GRID_SEARCH)
- heterozygosity                                    Heterozygosity value used to compute prior likelihoods for any locus
- pcr_error_rate                                    The PCR error rate to be used for computing fragment-based likelihoods
- genotyping_mode                                   Should we output confident genotypes (i.e. including ref calls) or just the variants? (DISCOVERY|GENOTYPE_GIVEN_ALLELES)
- output_mode                                       Should we output confident genotypes (i.e. including ref calls) or just the variants? (EMIT_VARIANTS_ONLY|EMIT_ALL_CONFIDENT_SITES|EMIT_ALL_SITES)
- standard_min_confidence_threshold_for_calling     The minimum phred-scaled confidence threshold at which variants not at 'trigger' track sites should be called
- standard_min_confidence_threshold_for_emitting    The minimum phred-scaled confidence threshold at which variants not at 'trigger' track sites should be emitted (and filtered if less than the calling threshold)
- noSLOD                                            If provided, we will not calculate the SLOD
- min_base_quality_score                            Minimum base quality required to consider a base for calling
- max_deletion_fraction                             Maximum fraction of reads with deletions spanning this locus for it to be callable [to disable, set to &lt; 0 or &gt; 1; default:0.05]
- min_indel_count_for_genotyping                    Minimum number of consensus indels required to trigger genotyping run
- indel_heterozygosity                              Heterozygosity for indel calling
- indelGapContinuationPenalty                       Indel gap continuation penalty
- indelGapOpenPenalty                               Indel gap open penalty
- indelHaplotypeSize                                Indel haplotype size
- doContextDependentGapPenalties                    Vary gap penalties by context
- indel_recal_file                                  Filename for the input covariates table recalibration .csv file - EXPERIMENTAL, DO NO USE
- indelDebug                                        Output indel debug info
- out                                               File to which variants should be written
- annotation                                        One or more specific annotations to apply to variant calls
- group                                             One or more classes/groups of annotations to apply to variant calls
-
-------
-
-**Citation**
-
-For the underlying tool, please cite `DePristo MA, Banks E, Poplin R, Garimella KV, Maguire JR, Hartl C, Philippakis AA, del Angel G, Rivas MA, Hanna M, McKenna A, Fennell TJ, Kernytsky AM, Sivachenko AY, Cibulskis K, Gabriel SB, Altshuler D, Daly MJ. A framework for variation discovery and genotyping using next-generation DNA sequencing data. Nat Genet. 2011 May;43(5):491-8. &lt;http://www.ncbi.nlm.nih.gov/pubmed/21478889&gt;`_
-
-If you use this tool in Galaxy, please cite Blankenberg D, et al. *In preparation.*
-
-  </help>
-</tool>