gatktools: variant_combine.xml comparison

comparison variant_combine.xml @ 15:01ff8dd37d4d draft default tip

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author	lz_hust
date	Sat, 01 Jun 2019 07:20:41 -0400
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+:01ff8dd37d4d
+<tool id="gatk2_variant_combine" name="Combine Variants" version="@VERSION@.0">
+<description></description>
+<macros>
+<import>gatk2_macros.xml</import>
+</macros>
+<expand macro="requirements" />
+<expand macro="version_command" />
+<command interpreter="python">
+gatk2_wrapper.py
+--stdout "${output_log}"
+#set $priority_order = []
+#for $input_variant in $reference_source.input_variants:
+-d "--variant:${input_variant.input_variant_name},%(file_type)s" "${input_variant.input_variant}" "${input_variant.input_variant.ext}" "input_variant_${input_variant.input_variant_name}"
+#set $input_variant_name = str( $input_variant.input_variant_name )
+#assert $input_variant_name not in $priority_order, "Variant Names must be unique" ##this should be handled by a validator
+#silent $priority_order.append( $input_variant_name )
+#end for
+-p '
+@JAR_PATH@
+-T "CombineVariants"
+--out "${output_variants}"
+\$GATK2_SITE_OPTIONS
+@THREADS@
+#if $reference_source.reference_source_selector != "history":
+-R "${reference_source.ref_file.fields.path}"
+#end if
+--genotypemergeoption "${genotype_merge_option}"
+--rod_priority_list "${ ','.join( $priority_order ) }"
+'
+#include source=$standard_gatk_options#
+##start analysis specific options
+#if $analysis_param_type.analysis_param_type_selector == "advanced":
+-p '
+--filteredrecordsmergetype "${analysis_param_type.filtered_records_merge_type}"
+${analysis_param_type.print_complex_merges}
+${analysis_param_type.filtered_are_uncalled}
+${analysis_param_type.minimal_vcf}
+${analysis_param_type.assume_identical_samples}
+#if str( $analysis_param_type.set_key ):
+--setKey "${analysis_param_type.set_key}"
+#end if
+--minimumN "${analysis_param_type.minimum_n}"
+'
+#end if
+</command>
+<inputs>
+<conditional name="reference_source">
+<expand macro="reference_source_selector_param" />
+<when value="cached">
+<repeat min="1" name="input_variants" title="Variants to Merge" help="Records will be prioritized in the order that you list them here (-V,--variant &amp;lt;variant&amp;gt;)">
+<param name="input_variant" type="data" format="vcf" label="Input variant file" />
+<param name="input_variant_name" type="text" value="" label="Variant name" help="Names must be unique">
+<validator type="length" min="1" message="You must provide a unique name for this set of variants" />
+</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_variants.input_variant" column="dbkey"/> -->
+</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 min="1" name="input_variants" title="Variants to Merge" help="Records will be prioritized in the order that you list them here (-V,--variant &amp;lt;variant&amp;gt;)">
+<param name="input_variant" type="data" format="vcf" label="Input variant file" />
+<param name="input_variant_name" type="text" value="" label="Variant name" help="Names must be unique">
+<validator type="length" min="1" message="You must provide a unique name for this set of variants" />
+</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>
+<param name="genotype_merge_option" type="select" label="How should we merge genotype records across records for samples shared across the ROD files" help="-genotypeMergeOptions,--genotypemergeoption &amp;lt;genotypemergeoption&amp;gt;" >
+<option value="UNIQUIFY" />
+<option value="PRIORITIZE" selected="true"/>
+<option value="UNSORTED" />
+<option value="REQUIRE_UNIQUE" />
+</param>
+<expand macro="gatk_param_type_conditional" />
+<expand macro="analysis_type_conditional">
+<param name="filtered_records_merge_type" type="select" label="How should we deal with records seen at the same site in the VCF, but with different FILTER fields?" help="-filteredRecordsMergeType,--filteredrecordsmergetype &amp;lt;filteredrecordsmergetype&amp;gt;" >
+<option value="KEEP_IF_ANY_UNFILTERED" selected="true"/>
+<option value="KEEP_IF_ALL_UNFILTERED" />
+</param>
+<param name="print_complex_merges" checked="false" type="boolean" truevalue="--printComplexMerges" falsevalue="" label="Print out interesting sites requiring complex compatibility merging" help="-printComplexMerges,--printComplexMerges" />
+<param name="filtered_are_uncalled" checked="false" type="boolean" truevalue="--filteredAreUncalled" falsevalue="" label="If true, then filtered VCFs are treated as uncalled, so that filtered set annotation don't appear in the combined VCF" help="-filteredAreUncalled,--filteredAreUncalled" />
+<param name="minimal_vcf" checked="false" type="boolean" truevalue="--minimalVCF" falsevalue="" label="If true, then the output VCF will contain no INFO or genotype INFO field" help="-minimalVCF,--minimalVCF" />
+<param name="set_key" type="text" value="" label="Key, by default set, in the INFO key=value tag emitted describing which set the combined VCF record came from." help="-setKey,--setKey &amp;lt;setKey&amp;gt;"/>
+<param name="assume_identical_samples" checked="false" type="boolean" truevalue="--assumeIdenticalSamples" falsevalue="" label="If true, assume input VCFs have identical sample sets and disjoint calls so that one can simply perform a merge sort to combine the VCFs into one, drastically reducing the runtime." help="-assumeIdenticalSamples,--assumeIdenticalSamples" />
+<param name="minimum_n" type="integer" value="1" label="Combine variants and output site only if variant is present in at least N input files." help="-minN,--minimumN &amp;lt;minimumN&amp;gt;"/>
+</expand>
+</inputs>
+<outputs>
+<data format="vcf" name="output_variants" label="${tool.name} on ${on_string} (variants)" />
+<data format="txt" name="output_log" label="${tool.name} on ${on_string} (log)" />
+</outputs>
+<tests>
+<test>
+<param name="reference_source_selector" value="history" />
+<param name="ref_file" value="phiX.fasta" ftype="fasta" />
+<param name="input_variant" value="gatk/gatk_variant_annotator/gatk_variant_annotator_out_1.vcf" ftype="vcf" />
+<param name="input_variant_name" value="from_variant_annotator" />
+<param name="genotype_merge_option" value="PRIORITIZE" />
+<param name="gatk_param_type_selector" value="basic" />
+<param name="analysis_param_type_selector" value="basic" />
+<output name="output_variants" file="gatk/gatk_variant_combine/gatk_variant_combine_out_1.vcf" lines_diff="4" />
+<output name="output_log" file="gatk/gatk_variant_combine/gatk_variant_combine_out_1.log.contains" compare="contains" />
+</test>
+</tests>
+<help>
+**What it does**
+Combines VCF records from different sources; supports both full merges and set unions. Merge: combines multiple records into a single one; if sample names overlap then they are uniquified. Union: assumes each rod represents the same set of samples (although this is not enforced); using the priority list (if provided), emits a single record instance at every position represented in the rods.
+For more information on using the CombineVariants module, see this `tool specific page &lt;http://www.broadinstitute.org/gatk/gatkdocs/org_broadinstitute_sting_gatk_walkers_variantutils_CombineVariants.html&gt;`_.
+To learn about best practices for variant detection using GATK, see this `overview &lt;http://www.broadinstitute.org/gatk/guide/topic?name=best-practices&gt;`_.
+If you encounter errors, please view the `GATK FAQ &lt;http://www.broadinstitute.org/gatk/guide/topic?name=faqs&gt;`_.
+------
+**Inputs**
+GenomeAnalysisTK: CombineVariants accepts variant files as input.
+------
+**Outputs**
+The output is a combined vcf file.
+Go `here &lt;http://www.broadinstitute.org/gatk/guide/topic?name=intro&gt;`_ for details on GATK file formats.
+-------
+**Settings**::
+out                         File to which variants should be written
+genotypemergeoption         How should we merge genotype records for samples shared across the ROD files? (UNIQUIFY|PRIORITIZE|UNSORTED|REQUIRE_UNIQUE)
+filteredrecordsmergetype    How should we deal with records seen at the same site in the VCF, but with different FILTER fields? KEEP_IF_ANY_UNFILTERED PASSes the record if any record is unfiltered, KEEP_IF_ALL_UNFILTERED requires all records to be unfiltered (KEEP_IF_ANY_UNFILTERED|KEEP_IF_ALL_UNFILTERED)
+rod_priority_list           When taking the union of variants containing genotypes: a comma-separated string describing the priority ordering for the genotypes as far as which record gets emitted; a complete priority list MUST be provided
+printComplexMerges          Print out interesting sites requiring complex compatibility merging
+filteredAreUncalled         If true, then filtered VCFs are treated as uncalled, so that filtered set annotation don't appear in the combined VCF
+minimalVCF                  If true, then the output VCF will contain no INFO or genotype INFO field
+setKey                      Key, by default set, in the INFO key=value tag emitted describing which set the combined VCF record came from.  Set to null if you don't want the set field emitted.
+assumeIdenticalSamples      If true, assume input VCFs have identical sample sets and disjoint calls so that one can simply perform a merge sort to combine the VCFs into one, drastically reducing the runtime.
+minimumN                    Combine variants and output site only if variant is present in at least N input files.
+@CITATION_SECTION@
+</help>
+<expand macro="citations" />
+</tool>

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comparison variant_combine.xml @ 15:01ff8dd37d4d draft default tip