annotate variant_eval.xml @ 0:fbca1c0956d2 draft default tip

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author devteam
date Tue, 01 Apr 2014 10:49:25 -0400
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1 <tool id="gatk_variant_eval" name="Eval Variants" version="0.0.8">
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2 <description></description>
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3 <requirements>
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4 <requirement type="package" version="1.4">gatk</requirement>
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5 </requirements>
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6 <macros>
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7 <import>gatk_macros.xml</import>
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8 </macros>
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9 <command interpreter="python">gatk_wrapper.py
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10 #from binascii import hexlify
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11 --max_jvm_heap_fraction "1"
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12 --stdout "${output_log}"
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13 #for $var_count, $variant in enumerate( $reference_source.variants ):
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14 -d "--eval:input_${var_count},%(file_type)s" "${variant.input_variant}" "${variant.input_variant.ext}" "input_variants_${var_count}"
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15 #end for
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16 -p 'java
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17 -jar "\$JAVA_JAR_PATH/GenomeAnalysisTK.jar"
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18 -T "VariantEval"
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19 --out "${output_report}"
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20 --num_threads \${GALAXY_SLOTS:-4}
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21 -et "NO_ET" ##ET no phone home
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22 ##-log "${output_log}" ##don't use this to log to file, instead directly capture stdout
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23 #if $reference_source.reference_source_selector != "history":
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24 -R "${reference_source.ref_file.fields.path}"
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25 #end if
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26 '
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27
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28 #for $rod_binding in $comp_rod_bind:
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29 -d "--comp:${rod_binding.comp_rod_name},%(file_type)s" "${rod_binding.comp_input_rod}" "${rod_binding.comp_input_rod.ext}" "input_comp_${rod_binding.comp_rod_name}"
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30 #if str( $rod_binding.comp_known_names ):
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31 -p '--known_names "${rod_binding.comp_rod_name}"'
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32 #end if
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33 #end for
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34
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35 #if str( $dbsnp_rod_bind_type.dbsnp_rod_bind_type_selector ) == 'set_dbsnp':
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36 -d "--dbsnp:${dbsnp_rod_bind_type.dbsnp_rod_name},%(file_type)s" "${dbsnp_rod_bind_type.dbsnp_input_rod}" "${dbsnp_rod_bind_type.dbsnp_input_rod.ext}" "input_dbsnp_${dbsnp_rod_bind_type.dbsnp_rod_name}"
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37 #if str( $dbsnp_rod_bind_type.dbsnp_known_names ):
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38 -p '--known_names "${dbsnp_rod_bind_type.dbsnp_rod_name}"'
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39 #end if
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40 #end if
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41
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42 #include source=$standard_gatk_options#
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43
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44
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45 ##start analysis specific options
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46 #if $analysis_param_type.analysis_param_type_selector == "advanced":
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47 #for $stratification in $analysis_param_type.stratifications:
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48 #set $select_string = "--select_exps '%s' --select_names '%s'" % ( str( $stratification.select_exps ), str( $stratification.select_name ) )
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49 -o '${ hexlify( $select_string ) }'
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50 #end for
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51 -p '
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52
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53 #for $sample in $analysis_param_type.samples:
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54 --sample "${sample.sample}"
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55 #end for
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56
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57 #if str( $analysis_param_type.stratification_modules ) != "None":
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58 #for $stratification_module in str( $analysis_param_type.stratification_modules).split( ',' ):
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59 --stratificationModule "${stratification_module}"
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60 #end for
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61 #end if
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62
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63 ${analysis_param_type.do_not_use_all_standard_stratifications}
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64
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65 #for $variant_type in $analysis_param_type.only_variants_of_type:
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66 --onlyVariantsOfType "${variant_type.variant_type}"
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67 #end for
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68
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69 #if str( $analysis_param_type.eval_modules ) != "None":
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70 #for $eval_module in str( $analysis_param_type.eval_modules).split( ',' ):
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71 --evalModule "${eval_module}"
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72 #end for
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73 #end if
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74
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75 ${analysis_param_type.do_not_use_all_standard_modules}
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76
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77 #if str( $analysis_param_type.num_samples ) != "0":
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78 --numSamples "${analysis_param_type.num_samples}"
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79 #end if
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80
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81 --minPhaseQuality "${analysis_param_type.min_phase_quality}"
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82
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83 #if str( $analysis_param_type.family ):
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84 --family_structure "${analysis_param_type.family}"
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85 #end if
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86
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87 --mendelianViolationQualThreshold "${analysis_param_type.mendelian_violation_qual_threshold}"
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88
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89 #if str( $analysis_param_type.ancestral_alignments ) != "None":
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90 --ancestralAlignments "${analysis_param_type.ancestral_alignments}"
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91 #end if
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92 '
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93 #if str( $analysis_param_type.known_cnvs ) != "None":
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94 -d "--knownCNVs" "${analysis_param_type.known_cnvs}" "${analysis_param_type.known_cnvs.ext}" "input_known_cnvs"
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95 #end if
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96
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97 #if str( $analysis_param_type.strat_intervals ) != "None":
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98 -d "--stratIntervals" "${analysis_param_type.strat_intervals}" "${analysis_param_type.strat_intervals.ext}" "input_strat_intervals"
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99 #end if
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100 #end if
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101 </command>
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102 <inputs>
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103
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104 <conditional name="reference_source">
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105 <expand macro="reference_source_selector_param" />
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106 <when value="cached">
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107 <repeat name="variants" title="Variant" min="1" help="-eval,--eval &amp;lt;eval&amp;gt;">
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108 <param name="input_variant" type="data" format="vcf" label="Input variant file" />
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109 </repeat>
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110 <param name="ref_file" type="select" label="Using reference genome" help="-R,--reference_sequence &amp;lt;reference_sequence&amp;gt;">
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111 <options from_data_table="gatk_picard_indexes">
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112 <!-- <filter type="data_meta" key="dbkey" ref="input_variant" column="dbkey"/> -->
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113 </options>
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114 <validator type="no_options" message="A built-in reference genome is not available for the build associated with the selected input file"/>
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115 </param>
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116 </when>
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117 <when value="history"> <!-- FIX ME!!!! -->
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118 <repeat name="variants" title="Variant" min="1" help="-eval,--eval &amp;lt;eval&amp;gt;">
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119 <param name="input_variant" type="data" format="vcf" label="Input variant file" />
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120 </repeat>
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121 <param name="ref_file" type="data" format="fasta" label="Using reference file" help="-R,--reference_sequence &amp;lt;reference_sequence&amp;gt;" />
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122 </when>
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123 </conditional>
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124
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125 <repeat name="comp_rod_bind" title="Binding for reference-ordered comparison data" help="-comp,--comp &amp;lt;comp&amp;gt;">
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126 <param name="comp_input_rod" type="data" format="vcf" label="Comparison ROD file" />
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127 <param name="comp_rod_name" type="text" value="Unnamed" label="Comparison ROD Name"/>
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128 <param name="comp_known_names" type="boolean" truevalue="--known_names" falsevalue="" label="Use Comparison ROD as known_names" help="-knownName,--known_names &amp;lt;known_names&amp;gt;"/>
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129 </repeat>
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130
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131 <conditional name="dbsnp_rod_bind_type">
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132 <param name="dbsnp_rod_bind_type_selector" type="select" label="Provide a dbSNP reference-ordered data file" help="-D,--dbsnp &amp;lt;dbsnp&amp;gt;">
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133 <option value="set_dbsnp" selected="True">Set dbSNP</option>
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134 <option value="exclude_dbsnp">Don't set dbSNP</option>
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135 </param>
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136 <when value="exclude_dbsnp">
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137 <!-- Do nothing here -->
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138 </when>
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139 <when value="set_dbsnp">
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140 <param name="dbsnp_input_rod" type="data" format="vcf" label="dbSNP ROD file" />
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141 <param name="dbsnp_rod_name" type="hidden" value="dbsnp" label="dbSNP ROD Name"/>
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142 <param name="dbsnp_known_names" type="boolean" truevalue="--known_names" falsevalue="" label="Use dbSNP ROD as known_names" help="-knownName,--known_names &amp;lt;known_names&amp;gt;" />
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143 </when>
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144 </conditional>
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145
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146 <expand macro="gatk_param_type_conditional" />
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147
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148
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149 <expand macro="analysis_type_conditional">
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150 <repeat name="stratifications" title="Stratification">
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151 <param name="select_exps" value="" type="text" label="Stratification Expression" help="-select,--select_exps &amp;lt;select_exps&amp;gt;">
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152 <sanitizer>
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153 <valid initial="string.printable">
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154 <remove value="&apos;"/>
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155 </valid>
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156 <mapping initial="none"/>
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157 </sanitizer>
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158 </param>
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159 <param name="select_name" value="" type="text" label="Name" help="-selectName,--select_names &amp;lt;select_names&amp;gt;"/>
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160 </repeat>
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161
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162 <repeat name="samples" title="Sample" help="-sn,--sample &amp;lt;sample&amp;gt;">
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163 <param name="sample" value="" type="text" label="Derive eval and comp contexts using only these sample genotypes, when genotypes are available in the original context"/>
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164 </repeat>
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165
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166 <param name="stratification_modules" type="select" multiple="True" display="checkboxes" label="Stratification modules to apply to the eval track(s)" help="-ST,--stratificationModule &amp;lt;stratificationModule&amp;gt;" >
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167 <!-- do these need individual options also? gatk wiki has little info -->
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168 <option value="AlleleFrequency" />
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169 <option value="AlleleCount" />
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170 <option value="CompRod" />
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171 <option value="Contig" />
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172 <option value="CpG" />
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173 <option value="Degeneracy" />
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174 <option value="EvalRod" />
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175 <option value="Filter" />
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176 <option value="FunctionalClass" />
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177 <option value="JexlExpression" />
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178 <option value="Sample" />
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179 <option value="IntervalStratification" />
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180 </param>
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181 <param name="do_not_use_all_standard_stratifications" checked="false" type="boolean" truevalue="--doNotUseAllStandardStratifications" falsevalue="" label="Do not use the standard stratification modules by default" help="-noST,--doNotUseAllStandardStratifications" />
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182
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183 <repeat name="only_variants_of_type" title="only Variants Of Type" help="--onlyVariantsOfType">
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184 <param name="variant_type" type="text" value="" label="only variants of these types will be considered during the evaluation"/>
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185 </repeat>
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186
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187 <param name="eval_modules" type="select" multiple="True" display="checkboxes" label="Eval modules to apply to the eval track(s)" help="-EV,--evalModule &amp;lt;evalModule&amp;gt;" >
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188 <!-- do these need individual options also? gatk wiki has little info -->
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189 <option value="ACTransitionTable" />
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190 <option value="AlleleFrequencyComparison" />
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191 <option value="AminoAcidTransition" />
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192 <option value="CompOverlap" />
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193 <option value="CountVariants" />
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194 <option value="GenotypeConcordance" />
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195 <option value="GenotypePhasingEvaluator" />
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196 <option value="IndelMetricsByAC" />
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197 <option value="IndelStatistics" />
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198 <option value="MendelianViolationEvaluator" />
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199 <option value="PrintMissingComp" />
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200 <option value="PrivatePermutations" />
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201 <option value="SimpleMetricsByAC" />
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202 <option value="ThetaVariantEvaluator" />
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203 <option value="TiTvVariantEvaluator" />
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204 <option value="VariantQualityScore" />
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205 </param>
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206 <param name="do_not_use_all_standard_modules" checked="false" type="boolean" truevalue="--doNotUseAllStandardModules" falsevalue="" label="Do not use the standard eval modules by default" help="-noEV,--doNotUseAllStandardModules" />
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207
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208 <param name="num_samples" type="integer" label="Number of samples (used if no samples are available in the VCF file" value="0" help="-ns,--numSamples &amp;lt;numSamples&amp;gt;"/>
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209 <param name="min_phase_quality" type="float" label="Minimum phasing quality " value="10.0" help="-mpq,--minPhaseQuality &amp;lt;minPhaseQuality&amp;gt;"/>
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210 <param name="family" type="text" value="" label="If provided, genotypes in will be examined for mendelian violations: this argument is a string formatted as dad+mom=child where these parameters determine which sample names are examined" help="--family_structure"/>
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211 <param name="mendelian_violation_qual_threshold" type="integer" label="Minimum genotype QUAL score for each trio member required to accept a site as a violation" value="50" help="-mvq,--mendelianViolationQualThreshold &amp;lt;mendelianViolationQualThreshold&amp;gt;"/>
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212 <param name="ancestral_alignments" type="data" format="fasta" optional="True" label="Fasta file with ancestral alleles" help="-aa,--ancestralAlignments &amp;lt;ancestralAlignments&amp;gt;" />
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213 <param name="known_cnvs" type="data" format="bed,gatk_interval,picard_interval_list" optional="True" label="File containing tribble-readable features describing a known list of copy number variants" help="-knownCNVs,--knownCNVs &amp;lt;knownCNVs&amp;gt;" />
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214 <param name="strat_intervals" type="data" format="bed,gatk_interval,picard_interval_list" optional="True" label="File containing tribble-readable features for the IntervalStratificiation" help="-stratIntervals,--stratIntervals &amp;lt;stratIntervals&amp;gt;" />
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215
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216 </expand>
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217
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218
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219 </inputs>
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220 <outputs>
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221 <data format="gatk_report" name="output_report" label="${tool.name} on ${on_string} (report)" />
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222 <data format="txt" name="output_log" label="${tool.name} on ${on_string} (log)" />
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223 </outputs>
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224 <tests>
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225 <test>
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226 <param name="reference_source_selector" value="history" />
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227 <param name="ref_file" value="phiX.fasta" ftype="fasta" />
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228 <param name="input_variant" value="gatk/gatk_variant_annotator/gatk_variant_annotator_out_1.vcf" ftype="vcf" />
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229 <param name="dbsnp_rod_bind_type_selector" value="set_dbsnp" />
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230 <param name="dbsnp_input_rod" value="gatk/fake_phiX_variant_locations.vcf" ftype="vcf" />
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231 <param name="dbsnp_known_names" value="True"/>
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232 <param name="comp_rod_bind" value="0" />
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233 <param name="gatk_param_type_selector" value="basic" />
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234 <param name="analysis_param_type_selector" value="basic" />
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235 <output name="output_report" file="gatk/gatk_variant_eval/gatk_variant_eval_out_1.gatk_report" />
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236 <output name="output_log" file="gatk/gatk_variant_eval/gatk_variant_eval_out_1.log.contains" compare="contains" />
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237 </test>
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238 </tests>
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239 <help>
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240 **What it does**
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241
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242 General-purpose tool for variant evaluation (% in dbSNP, genotype concordance, Ti/Tv ratios, and a lot more)
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243
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244 For more information on using the VariantEval module, see this `tool specific page &lt;http://www.broadinstitute.org/gsa/wiki/index.php/VariantEval&gt;`_.
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245
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246 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;`_.
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247
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248 If you encounter errors, please view the `GATK FAQ &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Frequently_Asked_Questions&gt;`_.
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249
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250 ------
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251
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252 **Inputs**
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253
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254 GenomeAnalysisTK: VariantEval accepts variant files as input.
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255
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256
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257 **Outputs**
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258
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259 The output is a table of variant evaluation.
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260
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261
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262 Go `here &lt;http://www.broadinstitute.org/gsa/wiki/index.php/Input_files_for_the_GATK&gt;`_ for details on GATK file formats.
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263
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264
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265 -------
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266
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267 **Settings**::
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268
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269 out An output file presented to the walker. Will overwrite contents if file exists.
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270 list List the available eval modules and exit
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271 select_exps One or more stratifications to use when evaluating the data
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272 select_names Names to use for the list of stratifications (must be a 1-to-1 mapping)
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273 sample Derive eval and comp contexts using only these sample genotypes, when genotypes are available in the original context
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274 known_names Name of ROD bindings containing variant sites that should be treated as known when splitting eval rods into known and novel subsets
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275 stratificationModule One or more specific stratification modules to apply to the eval track(s) (in addition to the standard stratifications, unless -noS is specified)
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276 doNotUseAllStandardStratifications Do not use the standard stratification modules by default (instead, only those that are specified with the -S option)
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277 onlyVariantsOfType If provided, only variants of these types will be considered during the evaluation, in
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278 evalModule One or more specific eval modules to apply to the eval track(s) (in addition to the standard modules, unless -noE is specified)
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279 doNotUseAllStandardModules Do not use the standard modules by default (instead, only those that are specified with the -E option)
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280 numSamples Number of samples (used if no samples are available in the VCF file
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281 minPhaseQuality Minimum phasing quality
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282 family_structure If provided, genotypes in will be examined for mendelian violations: this argument is a string formatted as dad+mom=child where these parameters determine which sample names are examined
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283 mendelianViolationQualThreshold Minimum genotype QUAL score for each trio member required to accept a site as a violation
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284 ancestralAlignments Fasta file with ancestral alleles
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285
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286 @CITATION_SECTION@
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287 </help>
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288 </tool>