Mercurial > repos > iuc > plink
view plink.xml @ 8:16d22eee0fe3 draft
"planemo upload for repository https://github.com/galaxyproject/tools-iuc/tree/master/tools/plink commit b63133897598f2881de7bad1f18fcd69d7d7e9df"
author | iuc |
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date | Thu, 02 Dec 2021 16:20:30 +0000 |
parents | 66b35562554d |
children | 272aca44b3dd |
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<tool id='plink' name='plink' version='@TOOL_VERSION@+galaxy@VERSION_SUFFIX@'> <macros> <token name='@TOOL_VERSION@'>1.9.b618</token> <token name='@VERSION_SUFFIX@'>3</token> <xml name='template_sanitizer'> <sanitizer> <valid initial='default'> <add value='#' /> <add value='@' /> <add value='$'/> <add value='['/> <add value=']'/> <add value='\'/> <remove value='"'/> <remove value='''/> </valid> </sanitizer> </xml> <xml name='chr_sanitizer'> <sanitizer> <valid initial='string.digits'> <add value='X' /> <add value='Y' /> <add value=' ' /> </valid> </sanitizer> </xml> <xml name='snp_sanitizer'> <sanitizer> <valid initial='string.ascii_letters + string.digits'/> </sanitizer> </xml> <xml name='snp_space_sanitizer'> <sanitizer> <valid initial='string.ascii_letters + string.digits'> <add value=' '/> </valid> </sanitizer> </xml> </macros> <xrefs> <xref type="bio.tools">plink</xref> </xrefs> <requirements> <requirement type='package' version='1.90b6.18'>plink</requirement> </requirements> <command detect_errors='exit_code'><![CDATA[ ## Create Plink folder for any inputs mkdir ./plink_output && mkdir ./plink_input ## If bmerge is set, create folder for merged files #if $functions.func == 'data_manage': #if $functions.bmerge.set == 'Yes': && mkdir bmerge_files && ln -s '$functions.bmerge.bed' bmerge_files/bmerge_input.bed && ln -s '$functions.bmerge.bim' bmerge_files/bmerge_input.bim && ln -s '$functions.bmerge.fam' bmerge_files/bmerge_input.fam #end if #end if #if $inputs.inputs.filetype == 'bfile': && ln -s '$inputs.inputs.bed' plink_input/plink_input.bed && ln -s '$inputs.inputs.bim' plink_input/plink_input.bim && ln -s '$inputs.inputs.fam' plink_input/plink_input.fam && plink --bfile plink_input/plink_input #elif $inputs.inputs.filetype == 'vcf': #if $inputs.inputs.input.is_of_type('bcf'): && plink --bcf '$inputs.inputs.input' #else: && plink --vcf '$inputs.inputs.input' #end if #end if ## Plink commands by section #if $inputs.covar_input: --covar '$inputs.covar_input' #end if #if $inputs.set_pheno.set_pheno == 'Yes': --pheno $inputs.set_pheno.pheno $inputs.set_pheno.all_pheno #end if #if $functions.func == 'filtering': ##ID list functions #if $functions.id_list.func == 'keep': --keep '$functions.id_list.file' #elif $functions.id_list.func == 'keep-fam': --keep-fam '$functions.id_list.file' #elif $functions.id_list.func == 'remove': --remove '$functions.id_list.file' #elif $functions.id_list.func == 'remove-fam': --remove-fam '$functions.id_list.file' #end if ##Extraction #if $functions.extraction.ex_func == 'extract': --extract $functions.extraction.range $functions.extraction.file #elif $functions.extraction.ex_func == 'exclude': --exclude $functions.extraction.range $functions.extraction.file #end if ##Chromosome-specificity #if $functions.chromosome: --chr $functions.chromosome #end if #if $functions.excluded_chromosome: --not-chr $functions.excluded_chromosome #end if $functions.extra_chromosomes #if $functions.autosome != 'none' $functions.autosome #end if ##SNP specificity #if $functions.snps_exclusives != 'No': --snps-only #if $functions.snps_exclusives == 'acgt': 'just-acgt' #end if #end if ##Variant windows #if $functions.ranges.single_multi == 'single': #if $functions.ranges.window.type == 'variant': #if $functions.ranges.window.from: --from $functions.ranges.window.from #end if #if $functions.ranges.window.to: --to $functions.ranges.window.to #end if #elif $functions.ranges.window.type == 'window': #if $functions.ranges.window.snp: --snp $functions.ranges.window.snp #end if #if $functions.ranges.window.exclude_snp: --exclude-snp $functions.ranges.window.exclude_snp #end if #if $functions.ranges.window.window: --window $functions.ranges.window.window #end if #else: #if $functions.ranges.window.from_bp: --from-bp $functions.ranges.window.from_bp #end if #if $functions.ranges.window.to_bp: --to-bp $functions.ranges.window.to_bp #end if #end if #elif $functions.ranges.single_multi == 'multi': $functions.ranges.force_intersect #if $functions.ranges.snps: --snps $functions.ranges.snps #end if #if $functions.ranges.exclude_snps: --exclude-snps $functions.ranges.exclude_snps #end if #end if ##Thinning #if $functions.thinning.thinning == 'Yes': #if $functions.thinning.thin: --thin $functions.thinning.thin #end if #if $functions.thinning.thin_count: --thin-count $functions.thinning.thin_count #end if #if $functions.thinning.bp_space: --bp-space $functions.thinning.bp_space #end if #if $functions.thinning.thin_indiv: --thin-indiv $functions.thinning.thin_indiv #end if #if $functions.thinning.thin_indiv_count: --thin-indiv-count $functions.thinning.thin_indiv_count #end if #end if ##Pheno/covariate ########### ########### ##Missing genotype rates #if $functions.geno_rates.geno: --geno $functions.geno_rates.geno #end if #if $functions.geno_rates.mind: --mind $functions.geno_rates.mind #end if ##Allele Frequencies #if $functions.allele_freq.maf: --maf $functions.allele_freq.maf #end if #if $functions.allele_freq.max_maf: --max-maf $functions.allele_freq.max_maf #end if #if $functions.allele_freq.mac: --mac $functions.allele_freq.mac #end if #if $functions.allele_freq.max_mac: --max-mac $functions.allele_freq.max_mac #end if ## Hardy-Weinberg #if $functions.hwe.hwe == 'Yes': --hwe $functions.hwe.hwe_val #for $type in $functions.hwe.modifiers: $type #end for #end if ##Sex and Founder filter #if $functions.sex_founder_filter.filter == 'Yes' $functions.sex_founder_filter.sex_select #if $functions.sex_founder_filter.no_sex_select: $functions.sex_founder_filter.no_sex_select #end if $functions.sex_founder_filter.nonfounders #end if #elif $functions.func == 'data_manage': #if $functions.bmerge.set == 'Yes': --bmerge bmerge_files/bmerge_input #end if #if $functions.template: --set-missing-var-ids $functions.template #end if $functions.recode #if $functions.flip: --flip $functions.flip #end if #if $functions.length: --new-id-max-allele-len $functions.length #end if #if $functions.update_cols.set == 'update_map': --update-map $functions.update_cols.input $functions.update_cols.col_num $functions.update_cols.old_col $functions.update_cols.skip #elif $functions.update_cols.set == 'update_name': --update-name $functions.update_cols.input $functions.update_cols.col_num $functions.update_cols.var_col $functions.update_cols.skip #end if #if $functions.ref_allele.set == 'yes': --reference-allele $functions.ref_allele.file $functions.ref_allele.column $functions.ref_allele.var_id $functions.ref_allele.skip #end if #if $functions.a2_allele.set == 'yes': --a2-allele $functions.a2_allele.file $functions.a2_allele.column $functions.a2_allele.var_id $functions.a2_allele.skip #end if #elif $functions.func == 'stats': $functions.freq $functions.hardy $functions.missing $functions.het #if $functions.sex.sex_stats: $functions.sex.sex_stats #if $functions.sex.mode: $functions.sex.mode.mode #if $functions.sex.mode.mode == 'ycount' $functions.sex.mode.female_max $functions.sex.mode.male_min $functions.sex.mode.female_max_obvs $functions.sex.mode.male_min_obvs #elif $functions.sex.mode.mode == 'y-only' $functions.sex.mode.female_max_obvs $functions.sex.mode.male_min_obvs #else: $functions.sex.mode.female_max $functions.sex.mode.male_min #end if #end if #end if #elif $functions.func == 'link': #if $functions.set_indep.choice == 'Yes': --indep-pairwise $functions.set_indep.window $functions.set_indep.step $functions.set_indep.r2 #end if ## #elif $functions.func == 'pair_compare': ## ## #elif $functions.func == 'dist_sim': ## #elif $functions.func == 'stratification': #if $functions.read_genome: --read-genome $functions.read_genome #end if #if $functions.cluster.cluster == 'Yes': --cluster #for $type in $functions.cluster.modifiers $type #end for #if $functions.cluster.mds.mds_scaling == 'Yes': --mds-plot $functions.cluster.mds.dimensions #for $type in $functions.cluster.mds.modifiers $type #end for #end if #end if #elif $functions.func == 'association': #if $functions.assoc.assoc == 'Yes': --assoc #if $functions.assoc.perm.perm == 'perm': perm #elif $functions.assoc.perm.perm == 'mperm': mperm='$functions.assoc.perm.value' #end if $functions.assoc.genedrop $functions.assoc.perm_count $functions.assoc.fisher $functions.assoc.count #end if #if $functions.adjust.adjust == 'Yes': --adjust #for $type in $functions.adjust.tests: $type #end for #end if ## #if $functions.linear.linear == 'Yes': ## --linear ## #if $functions.linear.perm == 'perm': ## perm ## #elif $functions.linear.perm == 'mperm': ## mperm='$functions.linear.perm.value' ## #end if ## $functions.linear.genedrop ## $functions.linear.perm_count ## $functions.linear.dominance ## $functions.linear.hide_covar ## $functions.linear.sex_covar ## $functions.linear.interaction ## $functions.linear.beta ## $functions.linear.standard_beta ## $functions.linear.intercept ## #end if #if $functions.logistic.logistic == 'Yes': --logistic #if $functions.logistic.perm.perm == 'perm': perm #elif $functions.logistic.perm.perm == 'mperm': mperm='$functions.logistic.perm.value' #end if $functions.logistic.genedrop $functions.logistic.perm_count $functions.logistic.dominance $functions.logistic.hide_covar $functions.logistic.sex_covar $functions.logistic.interaction $functions.logistic.beta $functions.logistic.intercept #end if --lambda $functions.lambda #elif $functions.func == 'ibd': #if $functions.genome.output_genome: --genome #for $type in $functions.genome.modifiers $type #end for #if $functions.genome.min: --min $functions.genome.min #end if #if $functions.genome.max: --max $functions.genome.max #end if #if $functions.genome.ppc: --ppc-gap $functions.genome.ppc #end if #end if ## #elif $functions.func == 'scoring': ## ## #else: ## --rerun $functions.logfile ## #end if --memory \${GALAXY_MEMORY_MB:-8192} --make-bed --out plink_output/plink_output #if $functions.func == 'association': #if $functions.logistic.logistic == 'Yes': && mkdir logistic_out && mv plink_output/plink_output.*.l* logistic_out && find ./logistic_out/. -type f -exec mv {} {}.txt ';' #end if #if $functions.adjust.adjust == 'Yes': && mkdir adjust_out && mv ./plink_output/*.adjuste* adjust_out && find ./adjust_out/. -type f -exec mv {} {}.txt ';' #end if #if $functions.assoc.assoc == 'Yes': && mkdir assoc_out && mv ./plink_output/*asso* assoc_out && find ./assoc_out/. -type f -exec mv {} {}.txt ';' #end if #end if ]]></command> <inputs> <section name='inputs' title='Data inputs' expanded='true'> <conditional name='inputs'> <param name='filetype' type='select' label='Main input data type'> <option value='bfile'>plink file</option> <option value='vcf'>VCF input file</option> </param> <when value='bfile'> <param format='pbed' name='bed' type='data' label='plink bed file'/> <param format='tabular,tsv' name='bim' type='data' label='plink bim file'/> <param format='txt' name='fam' type='data' label='plink fam file'/> </when> <when value='vcf'> <param name='input' format='vcf,vcf_bgzip,bcf' type='data' label='VCF/BCF Input file'/> </when> </conditional> <conditional name='set_pheno'> <param name='set_pheno' type='select' label='Set phenotype'> <option value=''>No</option> <option value='Yes'>Yes</option> </param> <when value=''/> <when value='Yes'> <param name='pheno' type='data' format='txt,tabular' label='Phenotype file' help='Read phenotype values from the 3rd column of the specified space- or tab-delimited file, instead of the .fam or .ped file.'/> <param name='all_pheno' type='boolean' truevalue='--all-pheno' falsevalue='' label='Allow all phenotypes present in the phenotype file to be subject to the association tests you have requested' checked='false'/> </when> </conditional> <param name='covar_input' type='data' format='tabular,tsv' label='Input covariate file' optional='true'/> </section> <conditional name='functions'> <param name='func' type='select' label='Plink functions'> <option value='filtering'>Filtering</option> <option value='data_manage'>Data Management</option> <option value='stats'>Basic statistics</option> <option value='link'>Linkage disequalibrium</option> <option value='stratification'>Population stratification</option> <option value='association'>Association analysis</option> <option value='ibd'>Identity-by-descent</option> <!-- <option value='rerun'>Rerun</option> --> </param> <when value='filtering'> <conditional name='id_list'> <param name='func' type='select' label='ID list functions'> <option value='none'>None</option> <option value='keep'>Keep by sample IDs</option> <option value='keep-fam'>Keep by family IDs</option> <option value='remove'>Remove by sample IDs</option> <option value='remove-fam'>Remove by family IDs</option> </param> <when value='none'/> <when value='keep'> <param format='tabular,tsv' name='file' type='data' label='Keep file.' help='Accepts one or more space/tab-delimited text files with sample IDs, and removes all unlisted samples from the current analysis;'/> </when> <when value='keep-fam'> <param format='tabular,tsv' name='file' type='data' label='Keep-fam file' help='Accepts text files with family IDs in the first column, and keeps entire families.'/> </when> <when value='remove'> <param format='tabular,tsv' name='file' type='data' label='Remove file' help='Accepts one or more space/tab-delimited text files with sample IDs, and removes all listed samples from the current analysis'/> </when> <when value='remove-fam'> <param format='tabular,tsv' name='file' type='data' label='Remove-fam file' help='Acceptz text files with family IDs in the first column, and removes entire families.'/> </when> </conditional> <conditional name='extraction'> <param name='ex_func' type='select' label='ID extraction functions'> <option value='none'>None</option> <option value='extract'>Keep by variant IDs</option> <option value='exclude'>Remove by variant IDs </option> </param> <when value='none'/> <when value='extract'> <param format='txt' name='file' type='data' label='Extract' help='Accepts one or more text file(s) with variant IDs , and removes all unlisted variants from the current analysis'/> <param type='boolean' name='range' truevalue='range' falsevalue='' help='Input file is input in set range format.'/> </when> <when value='exclude'> <param format='txt' name='file' type='data' label='Exclude' help='Accepts one or more text file(s) with variant IDs , and removes all listed variants from the current analysis'/> <param type='boolean' name='range' truevalue='range' falsevalue='' help='Input file is input in set range format.'/> </when> </conditional> <!-- <param name='border' type='integer' label='Bed border bp' help='Extends all the intervals in an input BED file (for e.g. extract bed0) by the given number of base-pairs on both sides.' optional='true'/> --> <!-- <conditional name='col-cond'> <param name='func' type='select' label='ID list functions'> <option value='none'/> <option value='extract-col-cond'/> <option value='extract-col-cond-match'/> <option value='extract-col-cond-mismatch'/> <option value='extract-col-cond-substr'/> <option value='extract-col-cond-min'/> <option value='extract-col-cond-max'/> </param> <when value='none'/> <when value='extract-col-cond'> </when> <when value='extract-col-cond-match'> </when> <when value='extract-col-cond-mismatch'> </when> <when value='extract-col-cond-substr'> </when> <when value='extract-col-cond-min'> </when> <when value='extract-col-cond-max'> </when> </conditional> --> <param name='chromosome' type='text' label='Chromosome(s)' help='Excludes all variants not on the listed chromosome(s). Can be listed as single chromsome, a hyphenated range, or comma separated list.' optional='true'> <expand macro='chr_sanitizer'/> </param> <param name='excluded_chromosome' type='text' label='Exclude Chromosome(s)' help='Excludes all variants on the listed chromosome(s). Can be listed as single chromsome, a hyphenated range, or comma separated list.' optional='true'> <expand macro='chr_sanitizer'/> </param> <param name='extra_chromosomes' type='boolean' truevalue='--aec' falsevalue='' checked='false' label='Allow extra chromosomes' help='Allows specified extra chromosomes/scaffolds not normally listed. ex. chr1_gl000191_random.'/> <param name='autosome' type='select' label='Autosome/unplaced exclusion'> <option value='none'>None</option> <option value='--autosome'>Exclude all unplaced and non-autosomal variants</option> <option value='--autosome-par'>Excludes all unplaced and non-autosomal variants, but keep XY/PAR1/PAR2. Can be combined with exclude-chromosmes.</option> </param> <param name='snps_exclusives' type='select' label='SNP exclusive'> <option value='No'>No</option> <option value='--snps-only'>Only return SNPs</option> <option value='acgt'>Return SNPs, excluding any other than {'A', 'C', 'G', 'T', 'a', 'c', 'g', 't', missing}</option> </param> <conditional name='ranges'> <param name='single_multi' type='select' label='Single or multiple variant-based range window?'> <option value=''>No range specified</option> <option value='single'>Single variants</option> <option value='multi'>Multiple variants</option> </param> <when value=''/> <when value='single'> <conditional name='window'> <param name='type' type='select' label='Specify range for variants'> <option value='variant'>Around/between specific variant(s)</option> <option value='window'>Around a specific variant</option> <option value='range'>Within a specific area (Must also specify a single chromosome in above input)</option> </param> <when value='variant'> <param name='from' type='text' label='From' help='Variant ID. Excludes all variants on different chromosomes than the named variant, as well as those with smaller base-pair position values. If they are used together but the --from variant is after the --to variant, they are automatically swapped.' optional='true'/> <param name='to' type='text' label='To' help='Variant ID. Excludes all variants on different chromosomes than the named variant, as well as those with larger base-pair position values. If they are used together but the --from variant is after the --to variant, they are automatically swapped.' optional='true'/> </when> <when value='window'> <param name='snp' type='text' label='SNP variant id to include' help='Use this OR SNP variant to exclude' optional='true'> <expand macro='snp_sanitizer'/> </param> <param name='exclude_snp' type='text' label='SNP variant id to exclude' help='Use this OR SNP variant to include' optional='true'> <expand macro='snp_sanitizer'/> </param> <param name='window' type='integer' label='Window' help='All variants with physical position no more than half the specified kb distance (decimal permitted) from the named variant are loaded as well' optional='true'/> </when> <when value='range'> <param name='from_bp' type='integer' label='from-bp' help='These flags let you use physical positions to specify a variant range to load. Must also have specified a chromosome in above settings.' optional='true'/> <param name='to_bp' type='integer' label='to-bp' help='These flags let you use physical positions to specify a variant range to load. Must also have specified a chromosome in above settings.' optional='true'/> </when> </conditional> </when> <when value='multi'> <param name='force_intersect' type='boolean' truevalue='--force-intersect' falsevalue='' label='Force intersect' help='To reduce the potential for confusion, PLINK 2 normally errors out when multiple variant-inclusion filters (--extract[-intersect], --extract-col-cond, --from/--to, --from-bp/--to-bp, --snp, --snps) are specified, since it may not be obvious whether the intersection or union will be taken. --force-intersect allows the run to proceed; the set intersection will be taken.'/> <param name='snps' type='text' label='List of SNP variant ids to include' optional='true'> <expand macro='snp_space_sanitizer'/> </param> <param name='exclude_snps' type='text' label='List of SNP variant ids to exclude' optional='true'> <expand macro='snp_space_sanitizer'/> </param> </when> </conditional> <conditional name='thinning'> <param name='thinning' type='select' label='Arbitrary thinning'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='thin' type='float' label='Thin' min='0' max='1.0' help='Removes variants at random by retaining each variant with probability p' optional='true'/> <param name='thin_count' type='integer' label='Thin Count' help='Removes variants at random until only n remain' min='1' optional='true'/> <param name='bp_space' type='integer' label='BP space' help='Excludes one variant from each pair closer than the given bp count' optional='true'/> <param name='thin_indiv' type='float' label='Thin Individual' min='0' max='1.0' help='Removes samples at random by retaining each sample with probability p' optional='true'/> <param name='thin_indiv_count' type='integer' label='Thin Individual count' min='1' help='Removes samples at random until only n remain.' optional='true'/> </when> </conditional> <!-- <conditional name='pheno_cov_based'> <param name='pheno_cov' type='select' label='Phenotype/Covariate-based'> <option value='No' selected='true'/> <option value='phenotype'/> <option value='Covariate'/> </param> <when value='No'/> <when value='phenotype'> --> <!-- keep-if <phenotype/covariate name> <operator> <value> remove-if <phenotype/covariate name> <operator> <value> require-pheno [phenotype name(s)...] keep-cats <filename> keep-cat-names <name(s)...> remove-cats <filename> remove-cat-names <name(s)...> keep-cat-pheno <phenotype/covariate name> remove-cat-pheno <phenotype/covariate name> </when> <when value='Covariate'> keep-if <phenotype/covariate name> <operator> <value> remove-if <phenotype/covariate name> <operator> <value> require-covar [covariate name(s)...] keep-cats <filename> keep-cat-names <name(s)...> remove-cats <filename> remove-cat-names <name(s)...> </when> </conditional> --> <section name='geno_rates' title='Missing Genotype Rates' expanded='true'> <param name='geno' type='float' min='0' max='1' label='Set Geno' help='filters out all variants with missing call rates exceeding the provided value (default 0.1) to be removed' optional='true'/> <param name='mind' type='float' min='0' max='1' label='Set Mind' help='filters out all samples with missing call rates exceeding the provided value (default 0.1) to be removed' optional='true'/> </section> <section name='allele_freq' title='Allele Frequencies' expanded='true'> <param name='maf' type='float' label='Minimum allele frequency' min='0' max='1.0' help='Filters out all variants with allele frequency below the provided threshold' optional='true'/> <param name='max_maf' type='float' label='Maximum allele frequency' min='0' max='1.0' help='Filters out all variants with allele frequency above the provided threshold' optional='true'/> <param name='mac' type='integer' label='Minimum allele count' min='1' help='Filters out all variants with allele counts below the provided threshold' optional='true'/> <param name='max_mac' type='integer' label='Maximum allele count' min='0' help='filters out all variants with allele counts above the provided threshold' optional='true'/> </section> <conditional name='hwe'> <param name='hwe' type='select' help='Set Hardy-Weinberg equilibrium tests'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='hwe_val' type='float' label='Hardy-Weinberg Equilibrium' help='Filters out all variants which have Hardy-Weinberg equilibrium exact test p-value below the provided threshold. It is recommended setting a low threshold—serious genotyping errors often yield extreme p-values like 1e-501 which are detected by any reasonable configuration of this test, while genuine SNP-trait associations can be expected to deviate slightly from Hardy-Weinberg equilibrium (so it is dangerous to choose a threshold that filters out too many variants).' value='1e-50' min='0' max='1'/> <param name='modifiers' type='select' label='Test modifiers' multiple='true' display='checkboxes' optional='true'> <option value='midp'>Apply the mid-p adjustment described in Graffelman J, Moreno V (2013) The mid p-value in exact tests for Hardy-Weinberg equilibrium</option> <option value='include-nonctrl'>Don't ignore cases and missing phenotypes'</option> </param> </when> </conditional> <conditional name='sex_founder_filter'> <param name='filter' type='select' label='Filter on sex and/or founders'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='sex_select' type='select' label='Sex select' help='Filter by phenotypes, experiment, and founder state.'> <option value=''>Do not specifically filter out based on sex or founders</option> <option value='--filter-cases'>Only include cases</option> <option value='--filter-controls'>Only include controls</option> <option value='--filter-males'>Only include males</option> <option value='--filter-females'>Only include females</option> <option value='--filter-founders'>Exclude all samples with at least one known parental ID</option> <option value='--filter-nonfounders'>Only include samples with at least one known parental ID</option> </param> <param name='no_sex_select' type='select' label='No sex settings' optional='true' help='How to deal with ambiguous sex phenotypes'> <option value=''>Change nothing with regards to ambiguous sex samples</option> <option value='--allow-no-sex'>Prevent samples with ambiguous sex frim having their phenotypes set to missing when analysis commands are run</option> <option value='--must-have-sex'>Force phenotypes of ambiguous-sex samples to missing in output</option> </param> <param name='nonfounders' type='boolean' label='Nonfouders' truevalue='--nonfounders' falsevalue='' checked='false' help='Include nonfounders in --freq[x] or --maf/--max-maf/--hwe calculations'/> </when> </conditional> </when> <when value='data_manage'> <conditional name='bmerge'> <param name='set' type='select' label='Merge plink tilesets'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param format='binary' name='bed' type='data' label='plink bed file'/> <param format='tabular,tsv' name='bim' type='data' label='plink bim file'/> <param format='tabular,tsv' name='fam' type='data' label='plink fam file'/> </when> </conditional> <param name='recode' type='boolean' label='Recode' truevalue='--recode' falsevalue='' checked='false' help='Create a new text fileset, after applying sample/variant filters and other operations'/> <param format='tsv,tabular' name='flip' type='data' label='Flip DNA strand for SNPs' help='Given a file containing a list of SNPs with A/C/G/T alleles, --flip swaps A↔T and C↔G.' optional='true'/> <param name='template' type='text' label='Update Variant Info: Template String' help='Replaces missing IDs. The parameter taken by these flags is a special template string, with a @ where the chromosome code should go, and a # where the base-pair position belongs.'> <expand macro='template_sanitizer'/> </param> <param name='length' type='integer' label='Max allele length' help='Length threshold to rename alleles. Recommended default is 23' optional='true'/> <conditional name='update_cols'> <param name='set' type='select' label='Update variant columns'> <option value='No'>No</option> <option value='update_map'>update-map</option> <option value='update_name'>update-name</option> </param> <when value='No'/> <when value='update_map'> <param name='input' type='data' format='tabular,tsv' help='By default, the new value is read from column 2 and the (old) variant ID from column 1, but you can adjust these positions with the second and third parameters.'/> <param name='col_num' type='integer' min='0' label='New ID column number' value='2'/> <param name='old_col' type='integer' min='0' label='Old ID column' value='1'/> <param name='skip' type='text' label='Skip' optional='true' help='Either a nonnegative integer, in which case it indicates the number of lines to skip at the top of the file, or a single nonnumeric character, which causes each line with that leading character to be skipped.'/> </when> <when value='update_name'> <param name='input' type='data' format='tabular,tsv' help='By default, the new value is read from column 2 and the (old) variant ID from column 1, but you can adjust these positions with the second and third parameters.'/> <param name='col_num' type='integer' min='0' label='BP column number' value='2'/> <param name='var_col' type='integer' min='0' label='Variant ID column' value='1'/> <param name='skip' type='text' label='Skip' optional='true' help='Either a nonnegative integer, in which case it indicates the number of lines to skip at the top of the file, or a single nonnumeric character, which causes each line with that leading character to be skipped.'/> </when> </conditional> <conditional name='ref_allele'> <param name='set' type='select' label='Set REF alleles' help='These cannot be used with any other commands.'> <option value='no'>No</option> <option value='yes'>Yes</option> </param> <when value='no'/> <when value='yes'> <param name='file' type='data' format='vcf' label='Set all alleles specified in the file to REF'/> <param name='column' type='integer' optional='true' min='1' label='Reference column number'/> <param name='var_id' type='integer' optional='true' min='1' label='Variant id column in file'/> <param name='skip' label='Skip' type='text' help='Either a nonnegative integer, in which case it indicates the number of lines to skip at the top of the file, or a single nonnumeric character, which causes each line with that leading character to be skipped.'/> </when> </conditional> <conditional name='a2_allele'> <param name='set' type='select' label='Set a2 alleles' help='These cannot be used with any other commands.'> <option value='no'>No</option> <option value='yes'>Yes</option> </param> <when value='no'/> <when value='yes'> <param name='file' type='data' format='vcf' label='Set all alleles specified in the file to first ALT allele'/> <param name='column' type='integer' value='4' optional='true' label='Alt column number'/> <param name='var_id' type='integer' value='3' optional='true' label='Variant id column in file'/> <param name='skip' label='Skip' type='boolean' truevalue='skip' falsevalue='' checked='false' help='Either a nonnegative integer, in which case it indicates the number of lines to skip at the top of the file, or a single nonnumeric character, which causes each line with that leading character to be skipped.'/> </when> </conditional> </when> <when value='stats'> <param name='freq' label='Return allele frequency file' type='boolean' truevalue='--freq' falsevalue=''/> <param name='hardy' label='Return Hardy-Weinberg statistics file' type='boolean' truevalue='--hardy' falsevalue='' help='Writes out writes autosomal Hardy-Weinberg equilibrium exact test statistics'/> <param name='missing' label='Missing Data' type='boolean' truevalue='--missing' falsevalue='' help='produces sample-based and variant-based missing data reports'/> <param name='het' label='Inbreeding' type='boolean' truevalue='--het' falsevalue='' help='Compute observed and expected homozygous/heterozygous genotype counts for each sample, and reports method-of-moments F coefficient estimates'/> <conditional name='sex'> <param name='sex_stats' label='Sex imputation' type='select'> <option value=''>No</option> <option value='--check-sex'>Compare sex assignments in input dataset with those imputed from X chromosome inbreeding coefficients</option> <option value='--impute-sex'> Changes sex assignments to the imputed values. Cannot be set with any other flags.</option> </param> <when value=''/> <when value='--check-sex'> <conditional name='mode'> <param name='mode' type='select' label='Mode select'> <option value=''>Base</option> <option value='ycount'>ycount</option> <option value='y-only'>y-only</option> </param> <when value=''> <param name='female_max' type='float' label='Female max proportion' min='0' max='1' optional='true'/> <param name='male_min' type='float' label='Male min proportion' min='0' max='1' optional='true'/> </when> <when value='ycount'> <param name='female_max' type='float' label='Female max proportion' min='0' max='1' optional='true'/> <param name='male_min' type='float' label='Male min proportion' min='0' max='1' optional='true'/> <param name='female_max_obvs' type='integer' label='Female max count' min='0' optional='true'/> <param name='male_min_obvs' type='integer' label='Male min count' min='0' optional='true'/> </when> <when value='y-only'> <param name='female_max_obvs' type='integer' label='Female max count' min='0' optional='true'/> <param name='male_min_obvs' type='integer' label='Male mincountn' min='0' optional='true'/> </when> </conditional> </when> <when value='--impute-sex'> <conditional name='mode'> <param name='mode' type='select' label='Mode select'> <option value=''>Base</option> <option value='ycount'>ycount</option> <option value='y-only'>y-only</option> </param> <when value=''> <param name='female_max' type='float' label='Female max proportion' min='0' max='1' optional='true'/> <param name='male_min' type='float' label='Male min proportion' min='0' max='1' optional='true'/> </when> <when value='ycount'> <param name='female_max' type='float' label='Female max proportion' min='0' max='1' optional='true'/> <param name='male_min' type='float' label='Male min proportion' min='0' max='1' optional='true'/> <param name='female_max_obvs' type='integer' label='Female max count' min='0' optional='true'/> <param name='male_min_obvs' type='integer' label='Male min count' min='0' optional='true'/> </when> <when value='y-only'> <param name='female_max_obvs' type='integer' label='Female max count' min='0' optional='true'/> <param name='male_min_obvs' type='integer' label='Male min count' min='0' optional='true'/> </when> </conditional> </when> </conditional> </when> <when value='link'> <conditional name='set_indep'> <param name='choice' label='Variant pruning' type='select' help='Since two-variant r2 only makes sense for biallelic variants, these collapse multiallelic variants down to most common allele vs. the rest.'> <option value='Yes'>Yes</option> <option value='No'>No</option> </param> <when value='No'/> <when value='Yes'> <param name='window' type='integer' label='Window size in bp' value='50' help='Window size'/> <param name='step' type='integer' label='Step size (variant ct)' value='5'/> <param name='r2' type='float' label='Unphased Hardcall r^2 Threshold' value='0.2' /> </when> </conditional> </when> <when value='stratification'> <param name='read_genome' label='Reusing an IBS/IBD calculation' format='tabular,tsv' type='data' optional='true'/> <conditional name='cluster'> <param name='cluster' type='select' help='Use IBS values calculated via --genome to perform complete linkage clustering'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='modifiers' type='select' label='Cluster flag modifiers' multiple='true' display='checkboxes' optional='true'> <option value='cc'>Prevent two all-case or two all-control clusters from being merged.</option> <option value='group-avg'>By default, the distance between two clusters is defined as the maximum pairwise distance between a member of the first cluster and a member of the second cluster. Cause average pairwise distance to be used instead.</option> <option value='missing'>Cause clustering to be based on identity-by-missingness</option> </param> <conditional name='mds'> <param name='mds_scaling' type='select' help='Return a Haploview-friendly multidimensional scaling report'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='dimensions' type='integer' label='Dimension count' value='10'/> <param name='modifiers' type='select' label='mds-plot flag modifiers' multiple='true' display='checkboxes' optional='true'> <option value='by-cluster'>Perform mds scaling on an inter-cluster distance matrix</option> <option value='eigendecomp'>Request faster eigendocomposition-based algorithm, yielding slightly different results</option> <option value='eigvals'>Write out top eigenvalues to separate file</option> </param> </when> </conditional> </when> </conditional> </when> <when value='association'> <conditional name='assoc'> <param name='assoc' label='Perform 1df chi-square allelic test' type='select'> <option value=''>No</option> <option value='Yes'>Yes</option> </param> <when value=''/> <when value='Yes'> <conditional name='perm'> <param name='perm' type='select' help='Request an adaptive or max(T) permutation test on the additive effect.'> <option value='No'>No</option> <option value='perm'>Perform Monte Carlo permutation test</option> <option value='mperm'>Perform a max(T) permutation test with specified number of replications</option> </param> <when value='No'/> <when value='perm'/> <when value='mperm'> <param name='value' label='Replications' type='integer' min='0' value='10000'/> </when> </conditional> <param name='genedrop' label='genedrop' type='boolean' truevalue='genedrop' falsevalue='' checked='false' help='Cause offspring genotypes to be regenerated via gene-dropping in the permutation test.'/> <param name='perm_count' label='Perm-count' type='boolean' truevalue='perm-count' falsevalue='' checked='false' help='Cause the permutation test report to include permutation counts instead of frequencies.'/> <param name='fisher' label='Fisher tests' type='select'> <option value=''>Don't specify</option> <option value='fisher'>Use fisher's exact test</option> <option value='fisher-midp'>User Fisher's exact test with Lancaster's mid-p adjustment</option> </param> <param name='count' label='Counts' type='boolean' truevalue='counts' falsevalue='' checked='false' help='Report allele counts instead of frequencies'/> </when> </conditional> <conditional name='adjust'> <param name='adjust' label='Report basic multiple testing corrections for the raw p-values' type='select'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <param name='tests' label='Testing modifiers' type='select' multiple='true' display='checkboxes' optional='true'> <option value='gc'>Use genomic-controlled p-values in the formulas</option> <option value='log10'>Replace the p-values in the .adjusted file with their negative base 10 logarithms.</option> <option value='qq-plot'>Add a quantile column to simplify QQ plotting.</option> </param> </when> </conditional> <!-- <conditional name='linear'> <param name='linear' type='select' label='Perform linenar regression and return report'> <option value='No'/> <option value='Yes'/> </param> <when value='No'/> <when value='Yes'> <conditional name='perm'> <param name='perm' type='select' help='Request an adaptive or max(T) permutation test on the additive effect.'> <option value='No'>No</option> <option value='perm'>Perform Monte Carlo permutation test</option> <option value='mperm'>Perform a max(T) permutation test with specified number of replications</option> </param> <when value='No'/> <when value='perm'/> <when value='mperm'> <param name='value' label='Replications' type='integer' min='0' value='10000'/> </when> </conditional> <param name='genedrop' label='genedrop' type='boolean' truevalue='genedrop' falsevalue='' checked='false' help='Cause offspring genotypes to be regenerated via gene-dropping in the permutation test.'/> <param name='perm_count' label='Perm-count' type='boolean' truevalue='perm-count' falsevalue='' checked='false' help='Cause the permutation test report to include permutation counts instead of frequencies.'/> <param name='set_test' label='set_test' type='boolean' truevalue='set-test' falsevalue='' checked='false' help='Test the significance of variant sets'/> <param name='dominance' label='Set dominance model' type='select'> <option value=''>Don't specify</option> <option value='genotypic'>Add an additive effect/dominance deviation 2df joint test (with two genotype-dependent variables in the regression, one with 0/1/2 coding and the second with 0/1/0</option> <option value='hethom'>Add an additive effect/dominance deviation 2df joint test (with two genotype-dependent variables in the regression, one with 0/0/1 coding and the second with 0/1/0</option> <option value='dominant'>Assume full dominance in A1 allele</option> <option value='recessive'>Assume full recessiveness in A1 allele</option> <option value='no-snp'>Request a regression only on the phenotype and the covariates, without reference to genomic data</option> </param> <param name='hide_covar' label='hide_covar' type='boolean' truevalue='hide-covar' falsevalue='' checked='false' help='Remove covariate-specific lines from the main report'/> <param name='sex_covar' label='Sex as a covariate' type='select'> <option value=''>Only used where specified</option> <option value='sex'>By default, when at least one male and one female is present, sex (male = 1, female = 0) is automatically added as a covariate on X chromosome SNPs, and nowhere else. The 'sex' modifier causes it to be added everywhere.</option> <option value='no-x-sex'>By default, when at least one male and one female is present, sex (male = 1, female = 0) is automatically added as a covariate on X chromosome SNPs, and nowhere else. The 'no-x-sex' modifier causes it to be excluded everywhere</option> </param> <param name='interaction' label='interaction' type='boolean' truevalue='interaction' falsevalue='' checked='false' help='Add genotype x covariate interactions to the model.'/> <param name='beta' label='beta' type='boolean' truevalue='beta' falsevalue='' checked='false' help=''/> <param name='standard_beta' label='standard-beta' type='boolean' truevalue='standard-beta' falsevalue='' checked='false' help=''/> <param name='intercept' label='intercept' type='boolean' truevalue='intercept' falsevalue='' checked='false' help=''/> </when> </conditional> --> <conditional name='logistic'> <param name='logistic' type='select' label='Perform logistic regression and return report'> <option value='No'>No</option> <option value='Yes'>Yes</option> </param> <when value='No'/> <when value='Yes'> <conditional name='perm'> <param name='perm' type='select' help='Request an adaptive or max(T) permutation test on the additive effect.'> <option value='No'>No</option> <option value='perm'>Perform Monte Carlo permutation test</option> <option value='mperm'>Perform a max(T) permutation test with specified number of replications</option> </param> <when value='No'/> <when value='perm'/> <when value='mperm'> <param name='value' label='Replications' type='integer' min='0' value='10000'/> </when> </conditional> <param name='genedrop' label='genedrop' type='boolean' truevalue='genedrop' falsevalue='' checked='false' help='Cause offspring genotypes to be regenerated via gene-dropping in the permutation test.'/> <param name='perm_count' label='Perm-count' type='boolean' truevalue='perm-count' falsevalue='' checked='false' help='Cause the permutation test report to include permutation counts instead of frequencies.'/> <param name='dominance' label='Set dominance model' type='select'> <option value=''>Don't specify</option> <option value='genotypic'>Add an additive effect/dominance deviation 2df joint test (with two genotype-dependent variables in the regression, one with 0/1/2 coding and the second with 0/1/0</option> <option value='hethom'>Add an additive effect/dominance deviation 2df joint test (with two genotype-dependent variables in the regression, one with 0/0/1 coding and the second with 0/1/0</option> <option value='dominant'>Assume full dominance in A1 allele</option> <option value='recessive'>Assume full recessiveness in A1 allele</option> <option value='no-snp'>Request a regression only on the phenotype and the covariates, without reference to genomic data</option> </param> <param name='hide_covar' label='Hide covar' type='boolean' truevalue='hide-covar' falsevalue='' checked='false' help='Remove covariate-specific lines from the main report'/> <param name='sex_covar' label='Sex as a covariate' type='select'> <option value=''>Only used where specified</option> <option value='sex'>By default, when at least one male and one female is present, sex (male = 1, female = 0) is automatically added as a covariate on X chromosome SNPs, and nowhere else. The 'sex' modifier causes it to be added everywhere.</option> <option value='no-x-sex'>By default, when at least one male and one female is present, sex (male = 1, female = 0) is automatically added as a covariate on X chromosome SNPs, and nowhere else. The 'no-x-sex' modifier causes it to be excluded everywhere</option> </param> <param name='interaction' label='Interaction' type='boolean' truevalue='interaction' falsevalue='' checked='false' help='Add genotype x covariate interactions to the model.'/> <param name='beta' label='Beta' type='boolean' truevalue='beta' falsevalue='' checked='false' help=''/> <param name='intercept' label='Intercept' type='boolean' truevalue='intercept' falsevalue='' checked='false' help=''/> </when> </conditional> <param name='lambda' type='float' label='Lambda value' optional='true'/> </when> <!-- <when value='scoring'> </when> --> <when value='ibd'> <conditional name='genome'> <param name='output_genome' type='select' help='Perform and return results of IBS/IBD computation'> <option value=''>No</option> <option value='Yes'>Yes</option> </param> <when value=''/> <when value='Yes'> <param name='min' type='float' label='min' min='0' max='1.0' help='Minimum PI_HAT value' optional='true'/> <param name='max' type='float' label='max' min='0' max='1.0' help='Maximum PI_HAT value' optional='true'/> <param name='ppc' type='integer' label='PPC-gap' min='0' help='Minimum distance between informative pairs of SNPs used in the pairwise population concordance (PPC) inn kbs' value='500' optional='true'/> <param name='modifiers' type='select' label='Genome flag modifiers' multiple='true' display='checkboxes' optional='true'> <option value='rel-check'>Remove pairs of samples with different FIDs</option> <option value='full'>Add IBS , HOMHOM and HETHET fields to output</option> <option value='unbounded'>Turn off clipping due to IBD estimator</option> <option value='nudge'>If PI_HAT2 greater than P(IBD=2), adjusts the final estimates to P(IBD=0) := (1-p2), P(IBD=1) := 2p(1-p), and P(IBD=2) := p2, where p is the current PI_HAT</option> </param> </when> </conditional> </when> <!-- <when value='rerun'> <param type='data' name='logfile' format='binary' label='Plink Log File'/> </when> --> </conditional> </inputs> <outputs> <!--Main--> <collection name='plink_out' type='list' label='Plink main outputs'> <data name='plink_bed' format='pbed' from_work_dir='plink_output/plink_output.bed'/> <data name='plink_bim' format='tabular' from_work_dir='plink_output/plink_output.bim'/> <data name='plink_fam' format='txt' from_work_dir='plink_output/plink_output.fam'/> <data name='plink_log' format='txt' from_work_dir='plink_output/plink_output.log'/> </collection> <!--Data Manage--> <data name='plink_ped' format='txt' from_work_dir='plink_output/plink_output.ped' label='${tool.name}: Recode ped'> <filter>functions['func'] == 'data_manage' and functions['recode']</filter> </data> <data name='plink_map' format='txt' from_work_dir='plink_output/plink_output.map' label='${tool.name}: Recode map'> <filter>functions['func'] == 'data_manage' and functions['recode']</filter> </data> <!--Stats--> <data name='frequency' format='tabular' from_work_dir='plink_output/plink_output.frq' label='${tool.name}: freq out'> <filter>functions['func'] == 'stats' and functions['freq']</filter> </data> <data name='hardy_out' format='tabular' from_work_dir='plink_output/plink_output.hwe' label='${tool.name}: Hardy-Weinberg equilibrium'> <filter>functions['func'] == 'stats' and functions['hardy']</filter> </data> <data name='missing_1' format='tabular' from_work_dir='plink_output/plink_output.imiss' label='${tool.name}: imiss'> <filter>functions['func'] == 'stats' and functions['missing']</filter> </data> <data name='missing_2' format='tabular' from_work_dir='plink_output/plink_output.lmiss' label='${tool.name}: lmiss'> <filter>functions['func'] == 'stats' and functions['missing']</filter> </data> <data name='het' format='tabular' from_work_dir='plink_output/plink_output.het' label='${tool.name}: Het'> <filter>functions['func'] == 'stats' and functions['het']</filter> </data> <data name='sex_check' format='tabular' from_work_dir='plink_output/plink_output.sexcheck' label='${tool.name}: Sex check'> <filter>functions['func'] == 'stats' and functions['sex']['sex_stats']</filter> </data> <!--Association--> <!--Assoc --> <collection name='assoc_outfiles' type='list' label='Association outfiles'> <discover_datasets directory='assoc_out' pattern='__name_and_ext__'/> <filter>functions['func'] == 'association' and functions['assoc']['assoc'] == 'Yes'</filter> </collection> <!--Adjust--> <collection name='adjust_outfiles' type='list' label='Adjust outfiles'> <discover_datasets directory='adjust_out' pattern='__name_and_ext__'/> <filter>functions['func'] == 'association' and functions['adjust']['adjust'] == 'Yes'</filter> </collection> <!--Logistic--> <collection name='log_outfiles' type='list' label='Logistic outfiles'> <discover_datasets directory='logistic_out' pattern='__name_and_ext__'/> <filter>functions['func'] == 'association' and functions['logistic']['logistic'] == 'Yes'</filter> </collection> <!--Link--> <data name='prune_in' format='tabular' from_work_dir='plink_output/plink_output.prune.in' label='${tool.name}: Prune In'> <filter>functions['func'] == 'link' and functions['set_indep']['choice'] == 'Yes'</filter> </data> <data name='prune_out' format='tabular' from_work_dir='plink_output/plink_output.prune.out' label='${tool.name}: Prune Out'> <filter>functions['func'] == 'link' and functions['set_indep']['choice'] == 'Yes'</filter> </data> <!--IBD--> <data name='genome' format='tabular' from_work_dir='plink_output/plink_output.genome' label='${tool.name}: Genome'> <filter>functions['func'] == 'ibd' and functions['genome']['output_genome']</filter> </data> <!--Stratifiction--> <data name='mds' format='txt' from_work_dir='plink_output/plink_output.mds' label='${tool.name}: MDS'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes' and functions['cluster']['mds']['mds_scaling'] == 'Yes'</filter> </data> <data name='cluster1' format='tabular' from_work_dir='plink_output/plink_output.cluster1' label='${tool.name}: Cluster 1'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes'</filter> </data> <data name='cluster2' format='tabular' from_work_dir='plink_output/plink_output.cluster2' label='${tool.name}: Cluster 2'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes'</filter> </data> <data name='cluster3' format='tabular' from_work_dir='plink_output/plink_output.cluster3' label='${tool.name}: Cluster 3'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes' and 'missing' not in functions['cluster']['modifiers']</filter> </data> <data name='cluster3missing' format='tabular' from_work_dir='plink_output/plink_output.cluster3.missing' label='${tool.name}: Cluster 3 missing'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes' and functions['cluster']['modifiers'] and 'missing' in functions['cluster']['modifiers']</filter> </data> <data name='mds_miss' format='tabular' from_work_dir='plink_output/plink_output.mdist.missing' label='${tool.name}: Mdist missing'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes' and functions['cluster']['modifiers'] and 'missing' in functions['cluster']['modifiers']</filter> </data> <data name='eigenvals' format='txt' from_work_dir='plink_output/plink_output.mds.eigvals' label='${tool.name}: Eigenvals'> <filter>functions['func'] == 'stratification' and functions['cluster']['cluster'] == 'Yes' and functions['cluster']['mds']['mds_scaling'] == 'Yes' and functions['cluster']['mds']['modifiers'] and 'eigvals' in functions['cluster']['mds']['modifiers']</filter> </data> </outputs> <tests> <test expect_num_outputs='5'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='filtering'/> <conditional name='id_list'> <param name='func' value='remove'/> <param name='file' value='1.tabular'/> </conditional> <conditional name='extraction'> <param name='ex_func' value='exclude'/> <param name='file' value='testing.txt'/> <param name='range' value='true'/> </conditional> <param name='snps_exclusives' value='--snps-only'/> <conditional name='ranges'> <param name='single_multi' value='single'/> <conditional name='window'> <param name='type' value='variant'/> <param name='from' value='snp0'/> <param name='to' value='snp3'/> </conditional> </conditional> <conditional name='thinning'> <param name='thinning' value='Yes'/> <param name='thin_count' value='4'/> </conditional> <section name='geno_rates'> <param name='geno' value='0.02'/> <param name='mind' value='0.02'/> </section> <section name='allele_freq'> <param name='maf' value='0.01'/> </section> <conditional name='hwe'> <param name='hwe' value='Yes'/> <param name='hwe_val' value='1e-50'/> <param name='modifiers' value='midp,include-nonctrl'/> </conditional> <conditional name='sex_founder_filter'> <param name='filter' value='Yes'/> <param name='sex_select' value='--filter-cases'/> <param name='no_sex_select' value='--allow-no-sex'/> <param name='nonfounders' value='--nonfounders'/> </conditional> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='test1_out.bed' compare='sim_size'/> <element name='plink_bim' file='test1_out.bim'/> <element name='plink_fam' file='test1_out.fam'/> </output_collection> </test> <test expect_num_outputs='7'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='data_manage'/> <conditional name='bmerge'> <param name='set' value='Yes'/> <param name='bed' value='plink_2.bed'/> <param name='bim' value='plink_2.bim'/> <param name='fam' value='plink_2.fam'/> </conditional> <param name='recode' value='--recode'/> <param name='template' value='@asd#123'/> <param name='length' value='23'/> <conditional name='update_cols'> <param name='set' value='update_name'/> <param name='input' value='update_cols.txt'/> <param name='col_num' value='1'/> <param name='var_col' value='2'/> <param name='skip' value='a'/> </conditional> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='test2_out.bed' compare='sim_size'/> <element name='plink_bim' file='test2_out.bim'/> <element name='plink_fam' file='test2_out.fam'/> </output_collection> <output name='plink_ped' file='out.ped'/> <output name='plink_map' file='out.map'/> </test> <test expect_num_outputs='5'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='vcf'/> <param name='input' value='test.vcf'/> </conditional> </section> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='vcf_out.bed'/> <element name='plink_bim' file='vcf_out.bim'/> <element name='plink_fam' file='vcf_out.fam'/> </output_collection> </test> <test expect_num_outputs='11'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='x_plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='stats'/> <param name='freq' value='--freq'/> <param name='hardy' value='--hardy'/> <param name='missing' value='--missing'/> <param name='het' value='--het'/> <conditional name='sex'> <param name='sex_stats' value='--check-sex'/> <conditional name='mode'> <param name='mode' value='ycount'/> <param name='female_max' value='0.2'/> <param name='male_min' value='0.8'/> <param name='female_max_obvs' value='10'/> <param name='male_min_obvs' value='200'/> </conditional> </conditional> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='stats.bed'/> <element name='plink_bim' file='stats.bim'/> <element name='plink_fam' file='stats.fam'/> <element name='plink_fam' file='stats.fam'/> </output_collection> <output name='frequency' file='out.freq'/> <output name='hardy_out' file='out.hardy'/> <output name='missing_1' file='out.imiss'/> <output name='missing_2' file='out.lmiss'/> <output name='het' file='out.het'/> <output name='sex_check' file='out.sexcheck'/> </test> <test expect_num_outputs='7'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='link'/> <conditional name='set_indep'> <param name='choice' value='Yes'/> <param name='window' value='51'/> <param name='step' value='6'/> <param name='r2' value='0.3'/> </conditional> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='test5_out.bed' compare='sim_size'/> <element name='plink_bim' file='test5_out.bim'/> <element name='plink_fam' file='test5_out.fam'/> </output_collection> <output name='prune_in' file='plink.prune.in'/> </test> <test expect_num_outputs='10'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='stratification'/> <param name='read_genome' value='plink.genome'/> <conditional name='cluster'> <param name='cluster' value='Yes'/> <param name='modifiers' value='cc,group-avg'/> <conditional name='mds'> <param name='mds_scaling' value='Yes'/> <param name='dimensions' value='10'/> <param name='modifiers' value='eigendecomp,eigvals'/> </conditional> </conditional> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='test6_out.bed' compare='sim_size'/> <element name='plink_bim' file='test6_out.bim'/> <element name='plink_fam' file='test6_out.fam'/> </output_collection> <output name='mds' value='plink.mds' compare='sim_size'/> <output name='cluster1' value='plink.cluster1' compare='sim_size'/> <output name='cluster2' value='plink.cluster2' compare='sim_size'/> <output name='cluster3' value='plink.cluster3' compare='sim_size'/> <output name='eigenvals' value='plink.mds.eigenval' compare='sim_size'/> </test> <test expect_num_outputs='8'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='association'/> <conditional name='assoc'> <param name='assoc' value='Yes'/> <conditional name='perm'> <param name='perm' value='mperm'/> <param name='value' value='10000'/> </conditional> <param name='fisher' value='fisher-midp'/> </conditional> <conditional name='adjust'> <param name='adjust' value='Yes'/> <param name='tests' value='gc,log10,qq-plot'/> </conditional> <conditional name='logistic'> <param name='logistic' value='Yes'/> <conditional name='perm'> <param name='perm' value='perm'/> </conditional> <param name='genedrop' value='genedrop'/> <param name='perm_count' value='perm-count'/> <param name='dominance' value='dominant'/> <param name='hide_covar' value='hide-covar'/> <param name='beta' value='beta'/> <param name='intercept' value='intercept'/> </conditional> <param name='lambda' value='1.0'/> </conditional> <output_collection name='plink_out' type='list'> <element name='plink_bed' file='out.assoc.bed' compare='sim_size'/> <element name='plink_bim' file='out.assoc.bim'/> <element name='plink_fam' file='out.assoc.fam'/> </output_collection> <output_collection name='assoc_outfiles' type='list' count='2'> <element name='plink_output.assoc.fisher.mperm' value='out.assoc.fisher.mperm' compare='sim_size'/> <element name='plink_output.assoc.fisher' value='out.assoc.fisher'/> </output_collection> <output_collection name='adjust_outfiles' type='list' count='1'> <element name='plink_output.assoc.fisher.adjusted' value='out.assoc.fisher.adjusted' compare='sim_size' /> </output_collection> <output_collection name='log_outfiles' type='list' count='3'> <element name='plink_output.assoc.logistic' value='out.assoc.logistic'/> <element name='plink_output.assoc.logistic.adjusted' value='out.assoc.logistic.adjusted'/> <element name='plink_output.assoc.logistic.perm' value='out.assoc.logistic.perm' compare='sim_size'/> </output_collection> </test> <test expect_num_outputs='6'> <section name='inputs'> <conditional name='inputs'> <param name='filetype' value='bfile'/> <param name='bed' value='plink.bed'/> <param name='bim' value='plink.bim'/> <param name='fam' value='plink.fam'/> </conditional> </section> <conditional name='functions'> <param name='func' value='ibd'/> <conditional name='genome'> <param name='output_genome' value='Yes'/> <param name='min' value='0.1'/> <param name='max' value='0.9'/> <param name='modifiers' value='full,unbounded,nudge'/> </conditional> </conditional> <output name='genome' file='out.genome'/> </test> </tests> <help><![CDATA[ PLINK is a free, open-source whole genome association analysis toolset, designed to perform a range of basic, large-scale analyses in a computationally efficient manner. For detailed usage notes, visit http://www.cog-genomics.org/plink/2.0/ ]]></help> <citations> <citation type='doi'>10.1186/s13742-015-0047-8</citation> </citations> </tool>