annotate pca_pipeline_def.xml @ 0:64e75e21466e draft default tip

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author pmac
date Wed, 01 Jun 2016 03:38:39 -0400
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1 <tool id="pca_pipeline" name="PCA Pipeline" version="1.0.0">
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2 <description>Iterative PCA pipeline</description>
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3 <requirements>
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4 <requirement type="package" version="2.8">Jinja2</requirement>
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5 <!--
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6 <requirement type="package" version="3.2.1">R</requirement>
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7 <requirement type="package" version="1.2.5">flashpcaR</requirement>
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8 -->
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9 </requirements>
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10 <command interpreter="python">
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11 <![CDATA[
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12 iterative_pca.py
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13 $datafile
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14 $data_type
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15 $iterations
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16 --sd_cutoff $sd_cutoff
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17 --absolute_prefix $output.files_path
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18 --html_file $output
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19 #if $control_tag
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20 --control_tag $control_tag
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21 #end if
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22 #if $cases_tag
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23 --cases_tag $cases_tag
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24 #end if
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25 #if $data_type.value == "variant_data"
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26 #if $user_configfile
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27 --config_file $user_configfile
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28 #else
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29 --config_file $cfile
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30 #end if
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31 #end if
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32 #if $clustering_flag.value == "yes"
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33 --clustering_flag
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34 --clustering_method $clustering_method
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35 --cluster_trimming $cluster_trimming
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36 #end if
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37 #if $ethnicity_file
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38 --ethnicity_file $ethnicity_file
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39 #end if
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40 #if $xsamples_file
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41 --reject_samples $xsamples_file
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42 #end if
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43 #if $xsnps_file
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44 --reject_snps $xsnps_file
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45 #end if
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46 --galaxy
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47 ]]>
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48 </command>
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49 <configfiles>
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50 <configfile name="cfile">#control
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51 control_tag,#Sample,$control_tag
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52 cases_tag,#Sample,$cases_tag
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53 #column_names
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54 genotype_column,$genotype_column
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55 reference_column,$reference_column
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56 alternate_column,$alternate_column
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57 sample_id_column,$sample_id_column
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58 chromosome_column,$chromosome_column
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59 position_column,$position_column
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60 variant_id_column,$variant_id_column
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61 #numeric_filters
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62 #for $i, $f in enumerate($numeric_filters)
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63 $f.filter_name,$f.column_name,$f.operation,$f.cutoff
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64 #end for
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65 #string_filters
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66 #for $i, $s in enumerate($string_filters)
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67 $s.filter_name,$s.column_name,$s.exact_flag,$s.accept_flag
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68 $(','.join($s.patterns.split('\n')))
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69 #end for</configfile>
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70 </configfiles>
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71 <inputs>
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72 <param name="datafile" type="data" label="Input datafile"/>
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73 <param name="data_type" type="select" label="Type of input data file">
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74 <option value="variant_data">Variant Data</option>
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75 <option value="numeric_ped">Numeric PED File</option>
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76 <option value="rdata">RData file</option>
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77 </param>
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78 <param name="iterations" type="integer" value="1" label="Number of iterations to complete"/>
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79 <param name="clustering_flag" type="select" display="radio" label="Do clustering?">
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80 <option value="yes">Yes</option>
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81 <option value="no">No</option>
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82 </param>
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83 <param name="clustering_method" type="select" label="Clustering method (ignore if you selected 'No' for 'Do clustering?')">
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84 <option value="dbscan">DBSCAN</option>
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85 <option value="hclust">Hierarchical Clustering</option>
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86 </param>
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87 <param name="cluster_trimming" type="select" label="Algorithm used to identify and remove cluster outliers (ignore if you selected 'No' for 'Do clustering?')">
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88 <option value="sd">Standard Deviations</option>
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89 <option value="mcd">Mean Cluster Distance</option>
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90 <option value="dbscan_outliers_only">DBSCAN outliers only (Only valid if DBSCAN is selected as 'Algorithm used to find clusters'</option>
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91 </param>
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92 <param name="sd_cutoff" type="float" value="2" label="Strictness of outlier trimming. Lower = more outliers cut at each stage, Higher = less outliers cut at each stage."/>
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93 <!-- Control and cases tag info -->
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94 <param name="control_tag" type="text" value="LP" label="Control Tag"/>
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95 <param name="cases_tag" type="text" value="HAPS" label="Cases Tag"/>
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96 <param name="user_configfile" type="data" format="txt" optional="true" label="Optional user provided config file.
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97 NB:
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98 - If this is set, ALL the fields below will be ignored.
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99 - If no input is provided, and the input data is a text file containing variant data, ALL the fields below except the filters MUST be filled in"/>
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100 <param name="ethnicity_file" type="data" format="txt" optional="true" label="Optional file containing data about ethnicity of samples"/>
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101 <param name="xsamples_file" type="data" format="txt" optional="true" label="Optional file containing EXACT ids of samples to exclude"/>
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102 <param name="xsnps_file" type="data" format="txt" optional="true" label="Optional file containing EXACT ids of SNPs to exclude"/>
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103 <!-- Column headers -->
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104 <param name="sample_id_column" type="text" value="#Sample" label="Sample ID Column"/>
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105 <param name="variant_id_column" type="text" value="ID" label="Variant ID Column"/>
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106 <param name="chromosome_column" type="text" value="CHROM" label="Chromosome Column"/>
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107 <param name="position_column" type="text" value="POS" label="Position Column"/>
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108 <param name="genotype_column" type="text" value="GT" label="Genotype Column"/>
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109 <param name="reference_column" type="text" value="REF" label="Reference Allele Column"/>
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110 <param name="alternate_column" type="text" value="ALT" label="Alternate Allele Column"/>
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111 <!-- Numeric Filters -->
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112 <repeat name="numeric_filters" title="Optional Numeric Filters">
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113 <param name="filter_name" type="text" label="Filter Name"/>
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114 <param name="column_name" type="text" label="Name of column to filter on"/>
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115 <param name="operation" type="select" label="Accept if column value is:">
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116 <option value="g">greater than</option>
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117 <option value="l">less than</option>
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118 <option value="e">equal to</option>
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119 <option value="ge">greater than or equal to</option>
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120 <option value="le">less than or equal to</option>
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121 </param>
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122 <param name="cutoff" type="float" value="0" label="Cutoff Value"/>
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123 </repeat>
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124 <!-- String Filters -->
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125 <repeat name="string_filters" title="Optional String Filters">
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126 <param name="filter_name" type="text" label="Filter Name"/>
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127 <param name="column_name" type="text" label="Name of column to filter on"/>
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128 <param name="exact_flag" type="select" label="Exact pattern matching?">
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129 <option value="exact">Yes</option>
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130 <option value="not_exact">No</option>
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131 </param>
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132 <param name="accept_flag" type="select" label="Action to perform after a successful match">
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133 <option value="accept">Accept</option>
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134 <option value="reject">Reject</option>
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135 </param>
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136 <param name="patterns" type="text" area="true" size="10x35" label="Patterns to match on" help="Enter a list of patterns here, separated by newlines"/>
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137 </repeat>
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138 </inputs>
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139 <outputs>
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140 <data name="output" format="html">
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141 <label>PCA summary: "${datafile.name}"</label>
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142 </data>
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143 </outputs>
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144 <help><![CDATA[
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145 .. class:: warningmark
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146
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147 '''WARNING''' This tool requires the 'dbscan' (https://cran.r-project.org/web/packages/dbscan/index.html) and 'flashpcaR' (https://github.com/gabraham/flashpca/releases) R packages to be installed on the galaxy instance.
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148
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149 ======================================
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150 Principle Component Analysis Pipeline
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151 ======================================
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152
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153 Overview
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154 --------
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155 A tool which performs iterative principle component analysis.
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156 The general idea is to seperate patient samples based on their ethnicity, by performing PCA on the variant data of each sample.
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157 After each analysis step, outliers are identified. The PCA is then repeated, with the outliers removed.
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158 This process continues for a set number of iterations specified by the user. After the pipeline completes, the user can see a
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159 detailed summary, as well as have access to the outliers identified at each iteration.
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160
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161 Primary Input
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162 ---------------
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163 As primary input the tools accepts a single file, which may be formatted in the following ways:
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164
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165 - **Variant data file:** This should be a tab-delimited text file, with each row containing data about a single variant site from a single person. If this option is selected, the column names which contain important information must also be specified, either via a configuration file (see below), or through the tool's form fields.
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166 - **Numeric ped file:** See http://pngu.mgh.harvard.edu/~purcell/plink/data.shtml for detailed information on PED format. This tool requires the affection status of each site to be specified numerically i.e.:
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167
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168 - 0 = homozygous reference
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169 - 1 = heterozygous
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170 - 2 = homozygous alternate
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171
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172 rather than consisting of pairs of genotypes for each site.
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173 - **RData file:** File containing stored data from an R session. For this tool the input must meet certain requirements:
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174
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175 - The file can only contain a SINGLE R object, which must be a list.
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176 - The list must contain a named 'bed' element.
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177 - The 'bed' element must be an n x m matrix/data frame, where n = number of samples, m = number of unique snps found in all the samples.
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178 - The A(i,j)th entry in the 'bed' matrix should indicate affectation status of the ith sample at the jth SNP site, according to the key for numeric ped files (as above).
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179 - The row names of the 'bed' matrix must contain the ids of the samples.
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180 - The column names of the 'bed' matrix must contain the ids of the SNPs.
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181
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182 If these very specific criteria are not met, the tool WILL fail.
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183
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184
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185
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186 Primary Output
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187 ---------------
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188
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189 HTML file containing plots of the PCA for each iteration.
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190 Possible plots, depending on user specified options:
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191
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192 - **Control vs Cases Plot:** If control and/or cases tags are provided, this plot will be output. ALL samples are plotted, with controls shown in blue, cases in red, unknown samples in black.
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193 - **Cluster Plot:** Output if user opts to do clustering. Samples are plotted, with clusters colour-coded. Outliers as identified by DBSCAN are always read and use an open circle as the icon. Trimmed clusters use a cross for the icon, instead of a circle. Both the outliers (open circles) AND the rejected clusters (crosses) will be dropped in the next iteration.
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194 - **Outliers Plot:** Output if user does NOT opt to do clustering. Samples which are considered outliers (as described above in 'Detecting outliers without clustering') are plotted as red open circles; all other samples are plotted as green full circles.
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195 - **Standard Deviations Plot:** Samples are colour-coded by standard deviation. Samples which fall within 1 standard devaiton of the median are red, <= 2 sds are green, <= 3 sds are blue, > 3 sds are purple.
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196 - **Ethnicity Plot:** Each ethnicity uses a specific colour and symbol. Fairly self-explanotory. Plot is only output if an ethnicity data file is provided as input.
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197
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198 Beneath the plots there are also two expandable lists. Samples excluded shows which samples were not part of the PCA for this iteration. This is cumulative. Outliers shows the outliers detected in THIS iteration. Any available data from the ethnicity file (if provided) is also displayed for each excluded sample.
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pmac
parents:
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199
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pmac
parents:
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200 Options/Secondary Inputs
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pmac
parents:
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201 ------------------------
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pmac
parents:
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202 - **Type of input data file:** Either a ped file or a text file as specified above
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pmac
parents:
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203 - **Number of iterations to complete:** A single iteration would involve performing PCA on the input data, then identifying and removing outliers. Two iterations would involve performing PCA again with the outliers identified from the first iteration excluded, three iterations would exclude the outliers from the first 2 stages, and so on and so forth.
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pmac
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204 - **Detecting outliers without clustering:** This is done by obtaining the standard deviations of the first two principle components. Any samples whose scores for either of these first two components falls more than 'n' number of standard deviations away from the component median are considered outliers.
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pmac
parents:
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205 - **Clustering:** The user may select from a range of algorithms which will try to identify clusters in the data, with each cluster hopefully corresponding to an ethnic group.
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pmac
parents:
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206 - **Clustering methods:**
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pmac
parents:
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207
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pmac
parents:
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208 - *DBSCAN (Density based spatial clustering of applications with noise):*
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pmac
parents:
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209
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pmac
parents:
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210 Forms clusters based on density of points, and does not require the number of clusters to be specified beforehand. Good for irregularly shaped, non-spherical clusters. Does NOT require all points to be part of clusters, and produces a set of 'outliers', i.e. points which do not belong to any clusters.
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pmac
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211
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pmac
parents:
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212 - *Hierarchical Clustering:*
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pmac
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213
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pmac
parents:
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214 Forms clusters based on distance between points. Tends to result in spherical clusters, but able to handle clusters of varying density. Forces all points to be part of a single cluster. The number of clusters is determined seperately, using the silhouette scores of all the points as a heuristic.
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pmac
parents:
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215
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pmac
parents:
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216 - **Cluster trimming methods:** All these methods first involve finding the centres of each cluster.
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pmac
parents:
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217
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pmac
parents:
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218 - *Standard Deviations:*
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pmac
parents:
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219
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pmac
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220 If the centroid of a cluster lies more than ‘n’ standard deviations (n is passed in as a parameter by the user) from the centroid of the entire dataset in either the x or y directions, the entire cluster is cut. If DBSCAN is selected, the outliers it identifies are also cut.
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pmac
parents:
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221
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pmac
parents:
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222 - *Mean Cluster Distance:*
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pmac
parents:
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223
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pmac
parents:
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224 Obtain the average distance between clusters, done by computing the distance between all pairs of clusters and taking the mean. For each cluster, we also compute an average “isolation” value, which is the mean of the distances between that particular cluster and all other clusters. If a cluster’s isolation value is larger than the average cluster distance (multiplied by the strictness weighting), then that cluster is considered an outlier and cut from the next iteration. If DBSCAN is selected, the outliers it identifies are also cut.
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pmac
parents:
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225
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pmac
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226 - *DBSCAN outliers only:*
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pmac
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227
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pmac
parents:
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228 Only cut the points identified by the DBSCAN algorithm as not belonging to any cluster. No entire clusters are cut. Obviously this method is only applicable if DBSCAN is selected as the clustering method. THE TOOL WILL NOT RUN IF YOU SELECT THIS OPTION TOGETHER WITH 'Hierarchical Clustering' AS THE CLUSTERING METHOD.
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pmac
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229
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pmac
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230 - **Strictness:** A multiplier used to determine how 'strict' the outlier cutting methods are. For example, if strictness = 1, and we are not doing clustering, all points which lie more than 1 sd from the median are cut. If strictness = 2, all points which lie more than 2 sd from the median are cut, etc.
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pmac
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231
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pmac
parents:
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232 - **Control Tag:** A pattern present in the ids of all the control samples, e.g. "LP"
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pmac
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233
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pmac
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234 - **Cases Tag:** A pattern present in the ids of all the cases samples, e.g. "HAPS"
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pmac
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235
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pmac
parents:
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236 - **Configuration file:** A configuration file to accompany an input variant text file. The config file has a rather specific format, an example is given below::
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pmac
parents:
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237
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pmac
parents:
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238 #control
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pmac
parents:
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239 control_tag,#Sample,HAPS
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pmac
parents:
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240 cases_tag,#Sample,LP
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pmac
parents:
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241 #column_names
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pmac
parents:
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242 genotype_column,GT
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pmac
parents:
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243 reference_column,REF
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pmac
parents:
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244 alternate_column,ALT
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pmac
parents:
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245 sample_id_column,#Sample
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pmac
parents:
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246 chromosome_column,CHROM
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pmac
parents:
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247 position_column,POS
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pmac
parents:
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248 variant_id_column,ID
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pmac
parents:
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249 #numeric_filters
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pmac
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250 strand_bias_filter,Fraction_with_strand_bias,<,0.03
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pmac
parents:
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251 position_bias_filter,Fraction_with_positional_bias,<,0.03
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pmac
parents:
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252 count_filter,Num_samples_variant,>,1
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pmac
parents:
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253 pass_filter,Fraction_samples_passed_filter,>,0.9
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pmac
parents:
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254 #string_filters
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pmac
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255 variant_type_filter,Variant_Type,exact,accept
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pmac
parents:
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256 SNV
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pmac
parents:
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257 genotype_filter,GT,exact,accept
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pmac
parents:
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258 '0/1,'1/1
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pmac
parents:
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259
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pmac
parents:
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260 File consists of up to four sections, the starts of which are marked by lines beginning with an octothorpe.
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pmac
parents:
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261
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pmac
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262 - *'#control' section:* Indicates substrings found in ids of controls and cases
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pmac
parents:
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263 - *'#column_names' section:* This is the only required section. First column indicates what column name (in the variant text file) the second column specifies. The same keys i.e. left most column values, as shown in the example must be used, e.g. sample_id_column, the RHS column names must match the names in the variant data file. If using a generated config file, only modify the RHS column, and DO NOT REMOVE ANY rows from this section.
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pmac
parents:
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264 - *'#numeric_filters' section:* Each filter takes up a single line, and is seperated into 4 sections by commas.
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265
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pmac
parents:
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266 - Column 1: Name of the filter, which is arbitrary
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pmac
parents:
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267 - Column 2: The name of the column in the variant file to filter on. If this column is not found, a warning is displayed
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pmac
parents:
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268 - Column 3: The criteria of the filter which must be passed in order for us to accept a particular row. E.g. less than, greater than
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pmac
parents:
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269 - Column 4: The cutoff value to be compared against.
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pmac
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270
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pmac
parents:
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271 - *'#string_filters' section:* Each filter takes up two lines.
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pmac
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272
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pmac
parents:
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273 - Line 1, Column 1: Arbitrary filter name
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pmac
parents:
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274 - Line 1, Column 2: Column name to filter on
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pmac
parents:
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275 - Line 1, Column 3: Do the patterns have to be exact matches, or just a substrings? E.g. if pattern = "HAPS" and string being compared = "HAPS-909090", if exact was true this would not be a successfull match, whereas if not_exact was true it would be a match.
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pmac
parents:
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276 - Line 1, Column 4: What to do with the row if a successful match is detected, e.g. accept or reject
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pmac
parents:
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277 - Line 2: A comma seperated list of patterns to match on
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pmac
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278
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pmac
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279
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pmac
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280 - **Ethnicity file:** An ethnicity file containing ethnicity data, and possible other data, on the samples. Note this data is not used to sort the input and has no effect on the PCA itself. It is used only to label the results of the output.
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pmac
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281
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pmac
parents:
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282 Requirements:
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pmac
parents:
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283
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pmac
parents:
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284 - tab delimited
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pmac
parents:
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285 - Must have at least two columns
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pmac
parents:
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286 - First column has sample ID's
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pmac
parents:
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287 - Second column has ethnicities
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pmac
parents:
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288 - First row must be a header
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pmac
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289
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pmac
parents:
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290 First few lines of a correctly formatted ethnicity file given below::
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pmac
parents:
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291
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pmac
parents:
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292 IID population Halo1.or.2. BloodAge SalivaAge COB ethnicity
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pmac
parents:
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293 LP-10000001 AUSTRALIAN Halo2 - LP-BC 67 NA Australia australian
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pmac
parents:
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294 LP-10000003 AUSTRALIAN Halo1 45 NA Australia australian southern_european
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pmac
parents:
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295 LP-10000005 AUSTRALIAN Halo1 73 NA Australia australian southern_european
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pmac
parents:
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296 LP-10000008 EUROPE Halo1 54 NA South Eastern Europe south_east_european
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pmac
parents:
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297 LP-10000009 OTHER Halo1 65 NA Southern & East Africa jewish
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pmac
parents:
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298
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pmac
parents:
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299 - **Exclude samples file:** A text file containing exact ids of samples to exclude from the PCA.
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pmac
parents:
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300
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pmac
parents:
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301 Requirements:
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pmac
parents:
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302
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pmac
parents:
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303 - single column
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pmac
parents:
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304 - sample ids seperated by newlines
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pmac
parents:
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305 - one sample id per line
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pmac
parents:
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306
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pmac
parents:
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307 Example::
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pmac
parents:
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308
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pmac
parents:
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309 HAPS-90573
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pmac
parents:
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310 HAPS-90578R
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pmac
parents:
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311 HAPS-110542
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pmac
parents:
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312 HAPS-110605
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pmac
parents:
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313 HAPS-110620
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pmac
parents:
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314 HAPS-110638
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pmac
parents:
diff changeset
315 HAPS-110649
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pmac
parents:
diff changeset
316 HAPS-110668
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pmac
parents:
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317 HAPS-110799
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pmac
parents:
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318 HAPS-110813
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pmac
parents:
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319 HAPS-110959
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pmac
parents:
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320 HAPS-111186
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pmac
parents:
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321 HAPS-111298
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pmac
parents:
diff changeset
322 HAPS-111404
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pmac
parents:
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323 HAPS-111493
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pmac
parents:
diff changeset
324 HAPS-111512
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pmac
parents:
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325 HAPS-111538
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pmac
parents:
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326
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pmac
parents:
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327 - **Exclude SNPS file:** A text file containing exact ids of SNPs to exclude from the PCA.
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pmac
parents:
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328
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pmac
parents:
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329 Requirements:
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pmac
parents:
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330
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pmac
parents:
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331 - single column
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pmac
parents:
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332 - snp ids seperated by newlines
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pmac
parents:
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333 - one snp id per line
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pmac
parents:
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334
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pmac
parents:
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335 Example::
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pmac
parents:
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336
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pmac
parents:
diff changeset
337 rs72896283
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pmac
parents:
diff changeset
338 rs7534447
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pmac
parents:
diff changeset
339 rs4662775
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pmac
parents:
diff changeset
340 rs10932813
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pmac
parents:
diff changeset
341 rs10932816
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pmac
parents:
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342 rs12330369
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pmac
parents:
diff changeset
343 rs1802904
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pmac
parents:
diff changeset
344 rs10902762
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pmac
parents:
diff changeset
345 rs9996817
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pmac
parents:
diff changeset
346 rs6446393
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pmac
parents:
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347 rs871133
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pmac
parents:
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348 rs4301095
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pmac
parents:
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349 rs941849
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pmac
parents:
diff changeset
350 rs6917467
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pmac
parents:
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351 rs75834296
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pmac
parents:
diff changeset
352 rs142922667
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pmac
parents:
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353
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pmac
parents:
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354 - **Required Column Headers:** If a variant text file is the primary input, the following information MUST be provided, either through the config file, or by filling out the corresponding fields in the tool submission form.
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pmac
parents:
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355
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pmac
parents:
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356 - Sample IDs: Name of the column containing the sample ids
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pmac
parents:
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357 - Chromosome: Name of the column indicating what chromosome the SNP is found on
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pmac
parents:
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358 - Position: Name of the column indicating at which position on the chromosome the SNP is found
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pmac
parents:
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359 - Genotype: The genotype of the sample for this site
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pmac
parents:
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360 - Reference: The 'normal'/'common' genotype for this site
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pmac
parents:
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361 - Alternate: The alternate genotype for this site
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pmac
parents:
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362 - Variant IDs: Name of the column indicating the ID of the SNP
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pmac
parents:
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363
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pmac
parents:
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364 - **Numeric Filters:** See Configuration file section
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pmac
parents:
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365 - **String Filters:** See Configuration file section
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pmac
parents:
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366
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pmac
parents:
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367 Other Output
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pmac
parents:
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368 -------------
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pmac
parents:
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369
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pmac
parents:
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370 - Tool will output a root folder containing the HTML file and all the plots, placed in directories seperated by iteration.
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pmac
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371 - If the input data was a variant file, the output folder will also contain a numeric ped file, generated before the first iteration, as well as a config file. The config file is either the exact one passed in by the user, or one automatically generated from the form input, which can be used for future PCA runs.
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pmac
parents:
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372
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pmac
parents:
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373 ]]>
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pmac
parents:
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374
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pmac
parents:
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375
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pmac
parents:
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376 </help>
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pmac
parents:
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377 </tool>