/usr/bin/loki_ext is in loki 2.4.7.4-7.
This file is owned by root:root, with mode 0o755.
The actual contents of the file can be viewed below.
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 33 34 35 36 37 38 39 40 41 42 43 44 45 46 47 48 49 50 51 52 53 54 55 56 57 58 59 60 61 62 63 64 65 66 67 68 69 70 71 72 73 74 75 76 77 78 79 80 81 82 83 84 85 86 87 88 89 90 91 92 93 94 95 96 97 98 99 100 101 102 103 104 105 106 107 108 109 110 111 112 113 114 115 116 117 118 119 120 121 122 123 124 125 126 127 128 129 130 131 132 133 134 135 136 137 138 139 140 141 142 143 144 145 146 147 148 149 150 151 152 153 154 155 156 157 158 159 160 161 162 163 164 165 166 167 168 169 170 171 172 173 174 175 176 177 178 179 180 181 182 183 184 185 186 187 188 189 190 191 192 193 194 195 196 197 198 199 200 201 202 203 204 205 206 207 208 209 210 211 212 213 214 215 216 217 218 219 220 221 222 223 224 225 226 227 228 229 230 231 232 233 234 235 236 237 238 239 240 241 242 243 244 245 246 247 248 249 250 251 252 253 254 255 256 257 258 259 260 261 262 263 264 265 266 267 268 269 270 271 272 273 274 275 276 277 278 279 280 281 282 283 284 285 286 287 288 289 290 291 292 293 294 295 296 297 298 299 300 301 302 303 304 305 306 307 308 309 310 311 312 313 314 315 316 317 318 319 320 321 322 323 324 325 326 327 328 329 330 331 332 333 334 335 336 337 338 339 340 341 342 343 344 345 346 347 348 349 350 351 352 353 354 355 356 357 358 359 360 361 362 363 364 365 366 367 368 369 370 371 372 373 | #!/usr/bin/perl
#
# Script to extract columns from loki.out
#
# Should work with output from all versions of Loki (up to loki_2.3)
#
# Simon Heath - September 2000
#
use Getopt::Std;
use IO::File;
use POSIX qw(tmpnam);
use strict;
my($i,$j,$k,%opt,$file,$hi,$lo,$flag,$out_type,$version,$link_fg,$start,$stop);
my($lg,%chrom,@map_start,@map_end,@map_length,$sex_map,$model);
my(@mkchrom,@mkpos,@mkname,$nmk,@col,$n_cov,$max_col,$ngroup);
my($it_col,$tv_col,$resvar_col,$mean_col,$addvar_col);
my($mean_set,$mean,$resvar_set,$resvar,$max_col1,$tau_col,$tau_beta,$tau,$tau_mode);
my($nc,$nqtl,$nqtl1,$line,$iter,$tv,$tv1,$sz,$nrand,@rand_col,@rand_fg,$tmp);
my(@no_output,$out_col_flag,$adj);
my($x1,$x2);
# Chromsome extracted defaults to the first one
$opt{c}=1;
getopts('xc:CDf:r:o:i:',\%opt);
# -r option sets a range of positions on the chromosome to look at
if($opt{r}) {
$tmp=$opt{r};
if($tmp=~/^([+-]?(?:(?:[0-9]*\.[0-9]+)|(?:[0-9]+))(?:[eE][-+]?[0-9]+)?)(.*)/) {
$lo=$1;
$tmp=$2;
}
if($tmp=~/^[,-:](.*)/) {
$tmp=$1;
if($tmp=~/^([+-]?(?:(?:[0-9]*\.[0-9]+)|(?:[0-9]+))(?:[eE][-+]?[0-9]+)?)/) {
$hi=$1;
}
}
die "Bad -r option\n" if(!defined($hi) && !defined($lo));
if(defined($lo) && defined($hi) && $lo>$hi) {
$tmp=$lo;
$lo=$hi;
$hi=$tmp;
}
}
# -i option sets a range of iterations to consider
if($opt{i}) {
$tmp=$opt{i};
if($tmp=~/^([1-9][0-9]*)(.*)/) {
$start=$1;
$tmp=$2;
}
if($tmp=~/^[,-:](.*)/) {
$tmp=$1;
if($tmp=~/^([1-9][0-9]*)/) {
$stop=$1;
}
}
die "Bad -i option\n" if(!defined($start) && !defined($stop));
if(defined($start) && defined($stop) && $start>$stop) {
$tmp=$start;
$start=$stop;
$stop=$tmp;
}
$start=1 if(!defined($start));
}
# Set default number of genetic groups
$ngroup=1;
# Used to store columns where to find interesting quantitities
# -1 means not known
$it_col=-1; # Iteration count
$tv_col=-1; # Total genetic variance
$resvar_col=-1; # Residual variance
$mean_col=-1; # Grand mean
$max_col=-1; # No. fixed output columns
$n_cov=-1; # No. covariate columns
$ngroup=1; # No. genetic groups
$tau_col=-1;
$tau_mode=-1;
$out_type=-1; # Output type
# Open output file if specified, otherwise we use STDOUT
if($opt{o}) {
open OFILE,">".$opt{o} or die "Couldn't open output file ",$opt{o},"\n";
} else {
open OFILE,">&STDOUT" or die "Couldn't dup STDOUT\n";
}
$sex_map=0;
$i=$opt{x}+$opt{C}+$opt{D};
die "Can not specify more that 1 of the options C,D,x at once.\n" if($i>1);
$opt{x}=1 unless $i;
$file=$opt{f}?$opt{f}:"loki.out";
open FILE,$file or die "Could not open file '$file'\n";
# Go though file
while(<FILE>) {
$line++;
if($flag) { # Parse the data portion of the file
split;
# Iteration number
$iter=$_[0];
if($opt{i}) {
next if($iter<$start);
last if(defined($stop) && $iter>$stop);
}
$nc=@_;
next if($nc<$max_col);
if($version==-1) {
$i=$max_col+$_[6];
last if($nc<$max_col);
$ngroup=$_[7];
} else {$i=$max_col;}
$max_col1=$i;
if($opt{C}) {
for($i=0;$i<$max_col1;$i++) {print OFILE " $_[$i]";}
print OFILE "\n";
next;
}
# Total variance
$tv1=0; #first get non-genetic variance
for($j=0;$j<$nrand;$j++) {
if($rand_fg[$j]==2) {
$sz=$_[$rand_col[$j]];
$tv1+=$sz;
}
}
# Now get genetic variance
if($tv_col>=0) {$tv=$_[$tv_col];}
else { # Not specified, must calculate
$tv=0;
for($j=0;$j<$nrand;$j++) {
$sz=$_[$rand_col[$j]];
$sz*=$sz if($rand_fg[$j]==1);
if($rand_fg[$j]!=2) {$tv+=$sz;}
}
}
# Count QTL's
$nqtl=0;
$nqtl1=0;
while($i<$nc) {
$lg=$_[$i];
die "Illegal linkage group $lg at line $line column ",$i+1,"\n" if($lg && !$chrom{$lg});
$i+=1+$sex_map if($lg || !$out_type);
$i+=4+$ngroup;
if($tv_col<0) {
$sz=$_[$i-1];
$tv+=$sz*$sz;
}
$nqtl++;
if($lg) {
$nqtl1++;
}
}
# If QTL numbers are given, check against what we found
if($out_type<2) {
die "Mismatch in QTL numbers ($nqtl,$_[1]) at line $line\n" if($nqtl!=$_[1]);
die "Mismatch in linked QTL numbers ($nqtl1,$_[2]) at line $line\n" if($nqtl1!=$_[2]);
}
# Get residual variance
if(!$resvar_set) {
# Do we know where it is ?
if($resvar_col>=0) {$resvar=$_[$resvar_col];}
# if not, guess
elsif($out_type<2) {$resvar=$_[4];}
else {$resvar=$_[2];}
}
# Total non-genetic variance
$tv1+=$resvar;
# Print out a 'standard' (across output types) set of columns
if($opt{D}) {
# Get Mean
if(!$mean_set) {
if($mean_col>=0) {$mean=$_[$mean_col];}
elsif($out_type<2) {$mean=$_[3];}
else {$mean=$_[1];}
}
# get Tau
if($tau_col>=0) {$tau=$_[$tau_col];}
elsif($tau_mode>=0) {
if($tau_mode==2) {$tau=$resvar*$tau_beta;}
else {$tau=$tau_beta;}
} else {
# Must be a very early version, assume that we know where tau is...
$tau=$_[5];
}
print OFILE "$iter $nqtl $nqtl1 $mean $resvar $tau ";
printf OFILE "%g",$tv;
# Are we on a recent version with all column info?
if($out_col_flag) {
for($i=1;$i<$max_col1;$i++) {
print OFILE " $_[$i]" if(!$no_output[$i]);
}
# This is more complicated
} else {
if(!$out_type) {$i=8;}
elsif($out_type<2) {$i=6;}
else {$i=3};
for(;$i<$max_col1;$i++) {
print OFILE " $_[$i]";
}
}
print OFILE "\n";
# Extract information about linked QTL's
} elsif($opt{x} && $nqtl) {
# Go through QTL's
$i=$max_col1;
while($i<$nc) {
$lg=$_[$i];
if($lg eq $opt{c}) {
$j=$i+1;
if($lg) {
$x1=$_[$j++];
$x2=$_[$j++] if($sex_map);
}
# Select QTL based on linkage group and range
if(!$lg || !$opt{r} || ((!defined($lo) || $x1>=$lo) && (!defined($hi) || $x1<=$hi))) {
print OFILE $iter;
# Print position if linked
if($lg) {
print OFILE " $x1";
print OFILE " $x2" if($sex_map);
}
for($k=0;$k<2+$ngroup;$k++) {print OFILE " ",$_[$j++];}
$sz=$_[$j];
print OFILE " $sz";
$sz*=$sz;
if($tv>0.0) {printf OFILE " %g",$sz/$tv;}
else {print OFILE " 0.0";}
if(($tv1+$tv)>0.0) {printf OFILE " %g\n",$sz/($tv+$tv1)}
else {print OFILE " 0.0\n";}
}
}
$i+=1+$sex_map if($lg || !$out_type);
$i+=4+$ngroup;
}
}
# We've reached the end of the header
} elsif(/^--*/) {
$flag=1;
# $max_col will not be set if working with an earlier version
if($max_col<0) {
# but $n_cov should be set unless ...
if($n_cov>=0) {
if($out_type<0) {$out_type=1;}
$max_col=3+$n_cov;
$version=1;
if(!$out_type) {$max_col+=5;}
elsif($out_type==1) {$max_col+=3;}
} else { # ... we are working with a genuine v2.0 copy
$out_type=0;
$max_col=8;
$version=-1;
}
}
} elsif(!$flag) { # First parse the header
if(/^Output format: (\d+)/) {
$out_type=$1;
next;
}
if(/^Created by loki (\d+).(\d+).(\d+).*:/) {
$version=2 if($1>2 || ($1==2 && $2>=3));
next;
}
# Pull out linkage group information if it is there
if(/^Linkage groups:$/) {
$link_fg=1;
next;
}
if($link_fg==1) {
# Check for linkage group names and map lengths
if(/(\d+): (.*)$/) {
$lg=$1;
if($2=~/^(.*) Map range: (.*)/) {
$chrom{$lg}=$1;
if($2=~/\((-?[0-9.]+)cM to (-?[0-9.]+)cM\)(.*)/) {
$map_start[$lg][0]=$1;
$map_end[$lg][0]=$1;
if($3=~/\((-?[0-9.]+)cM to (-?[0-9.]+)cM\)/) {
$map_start[$lg][1]=$1;
$map_end[$lg][1]=$1;
$sex_map=1;
}
} else { die "Error reading linkage group map range\n"; }
} else {$chrom{$lg}=$1;}
} elsif(/^\s+(.+) - ([\d\.]+)\s*([\d\.]*)/) {
if(!$opt{c} || $lg eq $opt{c}) {
$mkchrom[$nmk]=$lg;
$mkpos[$nmk][0]=$2;
$mkpos[$nmk][1]=$3;
$mkname[$nmk++]=$1;
}
} else {
# Check for total map length
if(/^Total Map Length: (.*)$/) {
if($1=~/(\d\d*\.?\d*)cM(.*)/) {
$map_length[0]=$1;
if($2=~/(\d\d*\.?\d*)cM$/) {
$map_length[1]=$1;
$sex_map=1;
}
} else { die "Error reading map lengths\n"; }
$link_fg=2;
next;
}
}
}
$model=$1 if(/^Model: (.+)/);
if($link_fg<3) {
if(/^Output columns:$/) {
$link_fg=3;
$out_col_flag=1;
next;
} elsif(/Output covariate data:$/) {
$link_fg=4;
}
} elsif($link_fg>2) {
if(/(\d+): (.*)/) {
$col[$1]=$2;
$tmp=$1-1;
if($link_fg==4) {
$link_fg=3;
if(!$tmp) {$adj=6;}
}
$tmp+=$adj;
if($2 eq "Total genetic variance") {
$tv_col=$tmp;
$no_output[$tmp]=1;
} elsif($2 eq "Additive variance") {
$rand_fg[$nrand]=0;
$rand_col[$nrand++]=$tmp;
} elsif($2=~/^Additional random variance for/) {
$rand_fg[$nrand]=2;
$rand_col[$nrand++]=$tmp;
} elsif($2=~/\S+ size$/) {
$rand_fg[$nrand]=1;
$rand_col[$nrand++]=$tmp;
} elsif($2 eq "Residual variance") {
$resvar_col=$tmp;
$no_output[$tmp]=1;
} elsif($2 eq "Grand mean") {
$mean_col=$tmp;
$no_output[$tmp]=1;
} elsif($2 eq "Tau") {
$tau_col=$tmp;
$no_output[$tmp]=1;
} elsif($2 eq "No. QTL's in model") {
$no_output[$tmp]=1;
} elsif($2 eq "No. linked QTL's") {
$no_output[$tmp]=1;
} elsif($2 eq "No. covariate columns") {
$no_output[$tmp]=1;
} elsif($2 eq "No. genetic groups") {
$no_output[$tmp]=1;
}
} elsif(/No. covariate columns: (\d+)/) {
$n_cov=$1;
} elsif(/No. fixed output columns: (\d+)/) {
$max_col=$1;
} elsif(/No. genetic groups: (\d+)/) {
$ngroup=$1;
} elsif(/^Sex specific map$/) {
$sex_map=1;
} elsif(/^Residual variance: ([0-9-.]+)/) {
$resvar_set=1;
$resvar=$1;
} elsif(/^Grand mean: ([0-9-.]+)/) {
$mean_set=1;
$mean=$1;
} elsif(/^Tau Mode: ([0-9]+)/) {
$tau_mode=$1;
} elsif(/^Tau Beta: ([0-9.]+)/) {
$tau_beta=$1;
}
}
}
}
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