Multiple platform build/check report for BioC 3.15 - CHECK results for atSNP on riesling1

Hostname	OS	Arch (*)	R version	Installed pkgs
nebbiolo1	Linux (Ubuntu 20.04.4 LTS)	x86_64	R Under development (unstable) (2022-02-17 r81757) -- "Unsuffered Consequences"	4334
riesling1	Windows Server 2019 Standard	x64	R Under development (unstable) (2021-11-21 r81221) -- "Unsuffered Consequences"	4097
palomino3	Windows Server 2022 Datacenter	x64	R Under development (unstable) (2022-02-17 r81757 ucrt) -- "Unsuffered Consequences"	4083
merida1	macOS 10.14.6 Mojave	x86_64	R Under development (unstable) (2022-03-02 r81842) -- "Unsuffered Consequences"	4134
Click on any hostname to see more info about the system (e.g. compilers) () as reported by 'uname -p', except on Windows and Mac OS X*

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###
### Running command:
###
###   D:\biocbuild\bbs-3.15-bioc\R\bin\R.exe CMD check --no-multiarch --install=check:atSNP.install-out.txt --library=D:\biocbuild\bbs-3.15-bioc\R\library --no-vignettes --timings atSNP_1.11.0.tar.gz
###
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* using log directory 'D:/biocbuild/bbs-3.15-bioc/meat/atSNP.Rcheck'
* using R Under development (unstable) (2021-11-21 r81221)
* using platform: x86_64-w64-mingw32 (64-bit)
* using session charset: ISO8859-1
* using option '--no-vignettes'
* checking for file 'atSNP/DESCRIPTION' ... OK
* checking extension type ... Package
* this is package 'atSNP' version '1.11.0'
* checking package namespace information ... OK
* checking package dependencies ... OK
* checking if this is a source package ... OK
* checking if there is a namespace ... OK
* checking for hidden files and directories ... OK
* checking for portable file names ... OK
* checking whether package 'atSNP' can be installed ... OK
* checking installed package size ... OK
* checking package directory ... OK
* checking 'build' directory ... OK
* checking DESCRIPTION meta-information ... OK
* checking top-level files ... OK
* checking for left-over files ... OK
* checking index information ... OK
* checking package subdirectories ... OK
* checking R files for non-ASCII characters ... OK
* checking R files for syntax errors ... OK
* checking whether the package can be loaded ... OK
* checking whether the package can be loaded with stated dependencies ... OK
* checking whether the package can be unloaded cleanly ... OK
* checking whether the namespace can be loaded with stated dependencies ... OK
* checking whether the namespace can be unloaded cleanly ... OK
* checking dependencies in R code ... NOTE
Namespaces in Imports field not imported from:
  'graphics' 'testthat'
  All declared Imports should be used.
* checking S3 generic/method consistency ... OK
* checking replacement functions ... OK
* checking foreign function calls ... OK
* checking R code for possible problems ... NOTE
ComputePValues: no visible binding for global variable 'motif'
ComputePValues: no visible binding for global variable 'snpid'
ComputePValues: no visible binding for global variable 'snpbase'
ComputePValues: no visible binding for global variable 'pval_ref'
ComputePValues: no visible binding for global variable 'pval_snp'
ComputePValues: no visible binding for global variable 'pval_cond_ref'
ComputePValues: no visible binding for global variable 'pval_cond_snp'
ComputePValues: no visible binding for global variable 'pval_diff'
ComputePValues: no visible binding for global variable 'pval_rank'
LoadSNPData: no visible global function definition for 'is'
LoadSNPData: no visible binding for global variable 'IUPAC_CODE_MAP'
MatchSubsequence: no visible binding for global variable 'motif'
MatchSubsequence: no visible binding for global variable 'snpid'
MatchSubsequence: no visible binding for global variable 'snpbase'
MatchSubsequence: no visible binding for global variable 'len_seq'
MatchSubsequence: no visible binding for global variable 'ref_seq'
MatchSubsequence : <anonymous>: no visible binding for global variable
  'motif'
checkMotifs: no visible global function definition for 'is'
checkSNPids: no visible global function definition for 'is'
dtMotifMatch: no visible binding for global variable 'ref_seq'
dtMotifMatch: no visible binding for global variable 'len_seq'
dtMotifMatch: no visible binding for global variable 'snp_ref_start'
dtMotifMatch: no visible binding for global variable 'ref_start'
dtMotifMatch: no visible binding for global variable 'snp_start'
dtMotifMatch: no visible binding for global variable 'snp_ref_end'
dtMotifMatch: no visible binding for global variable 'ref_end'
dtMotifMatch: no visible binding for global variable 'snp_end'
dtMotifMatch: no visible binding for global variable 'snp_ref_length'
dtMotifMatch: no visible binding for global variable
  'ref_aug_match_seq_forward'
dtMotifMatch: no visible binding for global variable
  'ref_aug_match_seq_reverse'
dtMotifMatch: no visible binding for global variable
  'snp_aug_match_seq_forward'
dtMotifMatch: no visible binding for global variable 'snp_seq'
dtMotifMatch: no visible binding for global variable
  'snp_aug_match_seq_reverse'
dtMotifMatch: no visible binding for global variable 'ref_strand'
dtMotifMatch: no visible binding for global variable 'ref_location'
dtMotifMatch: no visible binding for global variable 'snp_strand'
dtMotifMatch: no visible binding for global variable 'snp_location'
dtMotifMatch: no visible binding for global variable
  'ref_extra_pwm_left'
dtMotifMatch: no visible binding for global variable
  'ref_extra_pwm_right'
dtMotifMatch: no visible binding for global variable
  'snp_extra_pwm_left'
dtMotifMatch: no visible binding for global variable
  'snp_extra_pwm_right'
dtMotifMatch: no visible binding for global variable 'snpid'
match_subseq_par: no visible binding for global variable 'snpid'
match_subseq_par: no visible binding for global variable 'motif'
match_subseq_par: no visible binding for global variable 'snpbase'
match_subseq_par: no visible binding for global variable 'ref_strand'
match_subseq_par: no visible binding for global variable
  'ref_match_seq'
match_subseq_par: no visible binding for global variable 'ref_seq'
match_subseq_par: no visible binding for global variable 'ref_start'
match_subseq_par: no visible binding for global variable 'ref_end'
match_subseq_par: no visible binding for global variable 'ref_seq_rev'
match_subseq_par: no visible binding for global variable 'len_seq'
match_subseq_par: no visible binding for global variable 'snp_strand'
match_subseq_par: no visible binding for global variable
  'snp_match_seq'
match_subseq_par: no visible binding for global variable 'snp_seq'
match_subseq_par: no visible binding for global variable 'snp_start'
match_subseq_par: no visible binding for global variable 'snp_end'
match_subseq_par: no visible binding for global variable 'snp_seq_rev'
match_subseq_par: no visible binding for global variable
  'snp_seq_ref_match'
match_subseq_par: no visible binding for global variable
  'ref_seq_snp_match'
match_subseq_par: no visible binding for global variable 'motif_len'
match_subseq_par: no visible binding for global variable 'log_lik_ref'
match_subseq_par: no visible binding for global variable 'log_lik_snp'
match_subseq_par: no visible binding for global variable
  'log_lik_ratio'
match_subseq_par: no visible binding for global variable
  'log_enhance_odds'
match_subseq_par: no visible binding for global variable
  'log_reduce_odds'
match_subseq_par: no visible binding for global variable 'IUPAC'
motif_score_par: no visible binding for global variable 'motif'
motif_score_par: no visible binding for global variable 'snpbase'
plotMotifMatch: no visible global function definition for 'is'
results_motif_par: no visible binding for global variable 'p.value'
Undefined global functions or variables:
  IUPAC IUPAC_CODE_MAP is len_seq log_enhance_odds log_lik_ratio
  log_lik_ref log_lik_snp log_reduce_odds motif motif_len p.value
  pval_cond_ref pval_cond_snp pval_diff pval_rank pval_ref pval_snp
  ref_aug_match_seq_forward ref_aug_match_seq_reverse ref_end
  ref_extra_pwm_left ref_extra_pwm_right ref_location ref_match_seq
  ref_seq ref_seq_rev ref_seq_snp_match ref_start ref_strand
  snp_aug_match_seq_forward snp_aug_match_seq_reverse snp_end
  snp_extra_pwm_left snp_extra_pwm_right snp_location snp_match_seq
  snp_ref_end snp_ref_length snp_ref_start snp_seq snp_seq_ref_match
  snp_seq_rev snp_start snp_strand snpbase snpid
Consider adding
  importFrom("methods", "is")
to your NAMESPACE file (and ensure that your DESCRIPTION Imports field
contains 'methods').
* checking Rd files ... OK
* checking Rd metadata ... OK
* checking Rd cross-references ... OK
* checking for missing documentation entries ... OK
* checking for code/documentation mismatches ... OK
* checking Rd \usage sections ... OK
* checking Rd contents ... OK
* checking for unstated dependencies in examples ... OK
* checking contents of 'data' directory ... OK
* checking data for non-ASCII characters ... OK
* checking data for ASCII and uncompressed saves ... OK
* checking line endings in C/C++/Fortran sources/headers ... OK
* checking compiled code ... NOTE
Note: information on .o files for x64 is not available
File 'D:/biocbuild/bbs-3.15-bioc/R/library/atSNP/libs/x64/atSNP.dll':
  Found 'abort', possibly from 'abort' (C), 'runtime' (Fortran)
  Found 'exit', possibly from 'exit' (C), 'stop' (Fortran)
  Found 'printf', possibly from 'printf' (C)

Compiled code should not call entry points which might terminate R nor
write to stdout/stderr instead of to the console, nor use Fortran I/O
nor system RNGs. The detected symbols are linked into the code but
might come from libraries and not actually be called.

See 'Writing portable packages' in the 'Writing R Extensions' manual.
* checking files in 'vignettes' ... OK
* checking examples ... OK
Examples with CPU (user + system) or elapsed time > 5s
                  user system elapsed
ComputeMotifScore 0.80   0.03   10.72
ComputePValues    0.75   0.03   12.56
dtMotifMatch      0.68   0.00   11.63
MatchSubsequence  0.62   0.00   10.70
* checking for unstated dependencies in 'tests' ... OK
* checking tests ...
  Running 'test.R'
  Running 'test_change.R'
  Running 'test_diff.R'
  Running 'test_is.R'
 OK
* checking for unstated dependencies in vignettes ... OK
* checking package vignettes in 'inst/doc' ... OK
* checking running R code from vignettes ... SKIPPED
* checking re-building of vignette outputs ... SKIPPED
* checking PDF version of manual ... OK
* DONE

Status: 3 NOTEs
See
  'D:/biocbuild/bbs-3.15-bioc/meat/atSNP.Rcheck/00check.log'
for details.

Installation output

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###
### Running command:
###
###   D:\biocbuild\bbs-3.15-bioc\R\bin\R.exe CMD INSTALL atSNP
###
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* installing to library 'D:/biocbuild/bbs-3.15-bioc/R/library'
* installing *source* package 'atSNP' ...
** using staged installation
** libs
"C:/rtools40/mingw64/bin/"g++ -std=gnu++11  -I"D:/biocbuild/bbs-3.15-bioc/R/include" -DNDEBUG  -I'D:/biocbuild/bbs-3.15-bioc/R/library/Rcpp/include'   -I"C:/extsoft/include"     -O2 -Wall  -mfpmath=sse -msse2 -mstackrealign -fno-reorder-blocks-and-partition  -c ImportanceSample.cpp -o ImportanceSample.o
"C:/rtools40/mingw64/bin/"g++ -std=gnu++11  -I"D:/biocbuild/bbs-3.15-bioc/R/include" -DNDEBUG  -I'D:/biocbuild/bbs-3.15-bioc/R/library/Rcpp/include'   -I"C:/extsoft/include"     -O2 -Wall  -mfpmath=sse -msse2 -mstackrealign -fno-reorder-blocks-and-partition  -c ImportanceSampleChange.cpp -o ImportanceSampleChange.o
"C:/rtools40/mingw64/bin/"g++ -std=gnu++11  -I"D:/biocbuild/bbs-3.15-bioc/R/include" -DNDEBUG  -I'D:/biocbuild/bbs-3.15-bioc/R/library/Rcpp/include'   -I"C:/extsoft/include"     -O2 -Wall  -mfpmath=sse -msse2 -mstackrealign -fno-reorder-blocks-and-partition  -c ImportanceSampleDiff.cpp -o ImportanceSampleDiff.o
"C:/rtools40/mingw64/bin/"g++ -std=gnu++11  -I"D:/biocbuild/bbs-3.15-bioc/R/include" -DNDEBUG  -I'D:/biocbuild/bbs-3.15-bioc/R/library/Rcpp/include'   -I"C:/extsoft/include"     -O2 -Wall  -mfpmath=sse -msse2 -mstackrealign -fno-reorder-blocks-and-partition  -c MotifScore.cpp -o MotifScore.o
C:/rtools40/mingw64/bin/g++ -std=gnu++11 -shared -s -static-libgcc -o atSNP.dll tmp.def ImportanceSample.o ImportanceSampleChange.o ImportanceSampleDiff.o MotifScore.o -LC:/extsoft/lib/x64 -LC:/extsoft/lib -LD:/biocbuild/bbs-3.15-bioc/R/bin/x64 -lR
installing to D:/biocbuild/bbs-3.15-bioc/R/library/00LOCK-atSNP/00new/atSNP/libs/x64
** R
** data
** inst
** byte-compile and prepare package for lazy loading
** help
*** installing help indices
  converting help for package 'atSNP'
    finding HTML links ... done
    ComputeMotifScore                       html  
    ComputePValues                          html  
    GetIUPACSequence                        html  
    LoadFastaData                           html  
    LoadMotifLibrary                        html  
    LoadSNPData                             html  
    MatchSubsequence                        html  
    atSNP-package                           html  
    dtMotifMatch                            html  
    encode_motif                            html  
    encode_motifinfo                        html  
    jaspar_motif                            html  
    jaspar_motifinfo                        html  
    motif_library                           html  
    motif_match                             html  
    motif_scores                            html  
    plotMotifMatch                          html  
    prior                                   html  
    snpInfo                                 html  
    snp_tbl                                 html  
    transition                              html  
** building package indices
** installing vignettes
** testing if installed package can be loaded from temporary location
** testing if installed package can be loaded from final location
** testing if installed package keeps a record of temporary installation path
* DONE (atSNP)
Making 'packages.html' ...Warning in packageDescription(i, lib.loc = lib, fields = "Title", encoding = "UTF-8") :
  no package 'DiffBind' was found
 done

Tests output


R Under development (unstable) (2021-11-21 r81221) -- "Unsuffered Consequences"
Copyright (C) 2021 The R Foundation for Statistical Computing
Platform: x86_64-w64-mingw32/x64 (64-bit)

R is free software and comes with ABSOLUTELY NO WARRANTY.
You are welcome to redistribute it under certain conditions.
Type 'license()' or 'licence()' for distribution details.

R is a collaborative project with many contributors.
Type 'contributors()' for more information and
'citation()' on how to cite R or R packages in publications.

Type 'demo()' for some demos, 'help()' for on-line help, or
'help.start()' for an HTML browser interface to help.
Type 'q()' to quit R.

> library(atSNP)
> library(BiocParallel)
> library(testthat)
> 
> ## process the data
> data(example)
> 
> motif_scores <- ComputeMotifScore(motif_library, snpInfo, ncores = 1)
> 
> motif_scores <- MatchSubsequence(motif_scores$snp.tbl, motif_scores$motif.scores, ncores = 1, motif.lib = motif_library)
> 
> motif_scores[which(motif_scores$snpid == "rs7412" & motif_scores$motif == "SIX5_disc1"), ]
   snpid      motif
4 rs7412 SIX5_disc1
                                                        ref_seq
4 CTCCTCCGCGATGCCGATGACCTGCAGAAGCGCCTGGCAGTGTACCAGGCCGGGGCCCGCG
                                                        snp_seq motif_len
4 CTCCTCCGCGATGCCGATGACCTGCAGAAGTGCCTGGCAGTGTACCAGGCCGGGGCCCGCG        10
  ref_start ref_end ref_strand snp_start snp_end snp_strand log_lik_ref
4        29      38          -        22      31          +   -42.60672
  log_lik_snp log_lik_ratio log_enhance_odds log_reduce_odds      IUPAC
4    -38.4083     -4.198418           23.013       -2.917768 GARWTGTAGT
  ref_match_seq snp_match_seq ref_seq_snp_match snp_seq_ref_match snpbase
4    GCCAGGCGCT    CTGCAGAAGT        CTGCAGAAGC        GCCAGGCACT       T
> 
> len_seq <- sapply(motif_scores$ref_seq, nchar)
> snp_pos <- as.integer(len_seq / 2) + 1
> 
> i <- which(motif_scores$snpid == "rs7412" & motif_scores$motif == "SIX5_disc1")
> 
> test_that("Error: reference bases are not the same as the sequence matrix.", {
+   expect_equal(sum(snpInfo$sequence_matrix[31, ] != snpInfo$ref_base), 0)
+   expect_equal(sum(snpInfo$sequence_matrix[31, ] == snpInfo$snp_base), 0)
+ })
Test passed 
> 
> test_that("Error: log_lik_ratio is not correct.", {
+   expect_equal(motif_scores$log_lik_ref - motif_scores$log_lik_snp, motif_scores$log_lik_ratio)
+ })
Test passed 
> 
> test_that("Error: log likelihoods are not correct.", {
+ 
+   log_lik <- sapply(seq(nrow(motif_scores)),
+                         function(i) {
+                           motif_mat <- motif_library[[motif_scores$motif[i]]]
+                           colind<-which(snpInfo$snpids==motif_scores$snpid[i]) 
+                           bases <- snpInfo$sequence_matrix[motif_scores$ref_start[i]:motif_scores$ref_end[i], colind]
+                           if(motif_scores$ref_strand[i] == "-")
+                             bases <- 5 - rev(bases)
+                           log(prod(
+                                    motif_mat[cbind(seq(nrow(motif_mat)),
+                                                    bases)]))
+                         })
+ 
+   expect_equal(log_lik, motif_scores$log_lik_ref)
+ 
+   snp_mat <- snpInfo$sequence_matrix
+   snp_mat[cbind(snp_pos, seq(ncol(snp_mat)))] <- snpInfo$snp_base
+   log_lik <- sapply(seq(nrow(motif_scores)),
+                     function(i) {
+                       motif_mat <- motif_library[[motif_scores$motif[i]]]
+                       colind<-which(snpInfo$snpids==motif_scores$snpid[i])
+                       bases <- snp_mat[motif_scores$snp_start[i]:motif_scores$snp_end[i], colind]
+                       if(motif_scores$snp_strand[i] == "-")
+                         bases <- 5 - rev(bases)
+                       log(prod(
+                                motif_mat[cbind(seq(nrow(motif_mat)),
+                                                bases)]))
+                     })
+ 
+   expect_equal(log_lik, motif_scores$log_lik_snp)
+ })
Test passed 
> 
> test_that("Error: log_enhance_odds not correct.", {
+   
+   len_seq <- sapply(motif_scores$ref_seq, nchar)
+   snp_pos <- as.integer(len_seq / 2) + 1
+ 
+   ## log odds for reduction in binding affinity
+   
+   pos_in_pwm <- snp_pos - motif_scores$ref_start + 1
+   neg_ids <- which(motif_scores$ref_strand == "-")
+   pos_in_pwm[neg_ids] <- motif_scores$ref_end[neg_ids]- snp_pos[neg_ids] + 1
+   snp_base <- sapply(substr(motif_scores$snp_seq, snp_pos, snp_pos), function(x) which(c("A", "C", "G", "T") == x))
+   ref_base <- sapply(substr(motif_scores$ref_seq, snp_pos, snp_pos), function(x) which(c("A", "C", "G", "T") == x))
+   snp_base[neg_ids] <- 5 - snp_base[neg_ids]
+   ref_base[neg_ids] <- 5 - ref_base[neg_ids]
+   my_log_reduce_odds <- sapply(seq(nrow(motif_scores)),
+                                function(i)
+                                log(motif_library[[motif_scores$motif[i]]][pos_in_pwm[i], ref_base[i]]) -
+                                log(motif_library[[motif_scores$motif[i]]][pos_in_pwm[i], snp_base[i]])
+                                )
+ 
+   expect_equal(my_log_reduce_odds, motif_scores$log_reduce_odds)
+ 
+   ## log odds in enhancing binding affinity
+   
+   pos_in_pwm <- snp_pos - motif_scores$snp_start + 1
+   neg_ids <- which(motif_scores$snp_strand == "-")
+   pos_in_pwm[neg_ids] <- motif_scores$snp_end[neg_ids]- snp_pos[neg_ids] + 1
+   snp_base <- sapply(substr(motif_scores$snp_seq, snp_pos, snp_pos), function(x) which(c("A", "C", "G", "T") == x))
+   ref_base <- sapply(substr(motif_scores$ref_seq, snp_pos, snp_pos), function(x) which(c("A", "C", "G", "T") == x))
+   snp_base[neg_ids] <- 5 - snp_base[neg_ids]
+   ref_base[neg_ids] <- 5 - ref_base[neg_ids]
+   my_log_enhance_odds <- sapply(seq(nrow(motif_scores)),
+                                 function(i)
+                                 log(motif_library[[motif_scores$motif[i]]][pos_in_pwm[i], snp_base[i]]) -
+                                 log(motif_library[[motif_scores$motif[i]]][pos_in_pwm[i], ref_base[i]]) 
+                                )
+ 
+   expect_equal(my_log_enhance_odds, motif_scores$log_enhance_odds)
+   
+ 
+ })
Test passed 
> 
> test_that("Error: the maximum log likelihood computation is not correct.", {
+ 
+   snp_mat <- snpInfo$sequence_matrix
+   snp_mat[cbind(snp_pos, seq(ncol(snp_mat)))] <- snpInfo$snp_base
+ 
+   .findMaxLog <- function(seq_vec, pwm) {
+     snp_pos <- as.integer(length(seq_vec) / 2) + 1
+     start_pos <- snp_pos - nrow(pwm) + 1
+     end_pos <- snp_pos
+     rev_seq <- 5 - rev(seq_vec)
+     
+     maxLogProb <- -Inf
+     for(i in start_pos : end_pos) {
+       LogProb <- log(prod(pwm[cbind(seq(nrow(pwm)),
+                                     seq_vec[i - 1 + seq(nrow(pwm))])]))
+       if(LogProb > maxLogProb)
+         maxLogProb <- LogProb
+     }
+     for(i in start_pos : end_pos) {
+       LogProb <- log(prod(pwm[cbind(seq(nrow(pwm)),
+                                     rev_seq[i - 1 + seq(nrow(pwm))])]))
+       if(LogProb > maxLogProb)
+         maxLogProb <- LogProb
+     }
+     return(maxLogProb)
+   }
+   
+   ## find the maximum log likelihood on the reference sequence
+   my_log_lik_ref <- sapply(seq(nrow(motif_scores)),
+                            function(x) {
+ 		                         colind<-which(snpInfo$snpids==motif_scores$snpid[x])                           	
+                              seq_vec<- snpInfo$sequence_matrix[, colind]
+                              pwm <- motif_library[[motif_scores$motif[x]]]
+                              return(.findMaxLog(seq_vec, pwm))
+                            })
+ 
+   ## find the maximum log likelihood on the SNP sequence
+ 
+   my_log_lik_snp <- sapply(seq(nrow(motif_scores)),
+                            function(x) {
+                       		  colind<-which(snpInfo$snpids==motif_scores$snpid[x]) #ADDED
+                             seq_vec<- snp_mat[, colind]
+                             pwm <- motif_library[[motif_scores$motif[x]]]
+                             return(.findMaxLog(seq_vec, pwm))
+                            })
+   
+   expect_equal(my_log_lik_ref, motif_scores$log_lik_ref)
+   expect_equal(my_log_lik_snp, motif_scores$log_lik_snp)
+   
+ })
Test passed 
> 
> proc.time()
   user  system elapsed 
   8.46    0.79    9.23


R Under development (unstable) (2021-11-21 r81221) -- "Unsuffered Consequences"
Copyright (C) 2021 The R Foundation for Statistical Computing
Platform: x86_64-w64-mingw32/x64 (64-bit)

R is free software and comes with ABSOLUTELY NO WARRANTY.
You are welcome to redistribute it under certain conditions.
Type 'license()' or 'licence()' for distribution details.

R is a collaborative project with many contributors.
Type 'contributors()' for more information and
'citation()' on how to cite R or R packages in publications.

Type 'demo()' for some demos, 'help()' for on-line help, or
'help.start()' for an HTML browser interface to help.
Type 'q()' to quit R.

> library(atSNP)
> library(BiocParallel)
> library(testthat)
> data(example)
> 
> trans_mat <- matrix(rep(snpInfo$prior, each = 4), nrow = 4)
> test_pwm <- motif_library$SIX5_disc1
> scores <- as.matrix(motif_scores$motif.scores[3:4, 4:5])
> score_diff <- abs(scores[,2]-scores[,1])
> 
> pval_a <- .Call("test_p_value", test_pwm, snpInfo$prior, snpInfo$transition, scores, 0.15, 100)
> pval_ratio <- abs(log(pval_a[seq(nrow(scores)),1]) - log(pval_a[seq(nrow(scores)) + nrow(scores), 1]))
> 
> test_score <- test_pwm
> for(i in seq(nrow(test_score))) {
+   for(j in seq(ncol(test_score))) {
+     test_score[i, j] <- exp(mean(log(test_pwm[i, j] / test_pwm[i, -j])))
+   }
+ }
> 
> adj_mat <- test_pwm + 0.25
> motif_len <- nrow(test_pwm)
> 
> ## these are functions for this test only
> drawonesample <- function(theta) {
+     prob_start <- rev(rowSums(test_score ^ theta) / rowSums(adj_mat))
+     id <- sample(seq(motif_len), 1, prob = prob_start)
+     sample <- sample(1:4, 2 * motif_len - 1, replace = TRUE, prob = snpInfo$prior)
+     delta <- adj_mat
+     delta[motif_len - id + 1, ] <- test_score[motif_len - id + 1, ] ^ theta
+     sample[id - 1 + seq(motif_len)] <- apply(delta, 1, function(x) sample(seq(4), 1, prob = x))
+     ## compute weight
+     sc <- 0
+     for(s in seq(motif_len)) {
+       delta <- adj_mat
+       delta[motif_len + 1 - s, ] <- test_score[motif_len + 1 - s, ] ^ theta
+       sc <- sc + prod(delta[cbind(seq(motif_len), sample[s - 1 + seq(motif_len)])]) /
+         prod(snpInfo$prior[sample[s - 1 + seq(motif_len)]])
+     }
+     sample <- c(sample, id, sc)
+     return(sample)
+ }
> jointprob <- function(x) prod(test_pwm[cbind(seq(motif_len), x)])
> maxjointprob <- function(x) {
+   maxp <- -Inf
+   p <- -Inf
+   for(i in 1:motif_len) {
+     p <- jointprob(x[i:(i+motif_len - 1)])
+     if(p > maxp)
+       maxp <- p
+   }
+   for(i in 1:motif_len) {
+     p <- jointprob(5 - x[(i+motif_len - 1):i])
+     if(p > maxp)
+       maxp <- p
+   }
+   return(maxp)
+ }
> get_freq <- function(sample) {
+   emp_freq <- matrix(0, nrow = 2 * motif_len - 1, ncol = 4)
+   for(i in seq(2 * motif_len - 1)) {
+     for(j in seq(4)) {
+       emp_freq[i, j] <- sum(sample[i, ] == j - 1)
+     }
+   }
+   emp_freq <- emp_freq / rowSums(emp_freq)
+   return(emp_freq)
+ }
> 
> test_that("Error: quantile function computing are not equivalent.", {
+   for(p in c(0.01, 0.1, 0.5, 0.9, 0.99) ) {
+     delta <- .Call("test_find_percentile_change", score_diff, p, package = "atSNP")
+     delta.r <- as.double(sort(abs(scores[,2]-scores[,1]))[ceiling((1 - p) * (nrow(scores)))])
+     expect_equal(delta, delta.r)
+   }
+ })
Test passed 
> 
> test_that("Error: the scores for samples are not equivalent.", {
+   p <- 0.1
+   delta <- .Call("test_find_percentile_change", score_diff, p, package = "atSNP")
+   theta <- .Call("test_find_theta_change", test_score, adj_mat, delta, package = "atSNP")
+   ## Use R code to generate a random sample
+   for(i in seq(10)) {
+     sample <- drawonesample(theta)
+     sample_score <- .Call("test_compute_sample_score_change", test_pwm, test_score, adj_mat, sample[seq(2 * motif_len - 1)] - 1, snpInfo$prior, trans_mat, sample[2 * motif_len] - 1, theta, package = "atSNP")
+     expect_equal(sample[2 * motif_len + 1], sample_score[1])
+     sample1 <- sample2 <- sample3 <- sample
+     sample1[motif_len] <- seq(4)[-sample[motif_len]][1]
+     sample2[motif_len] <- seq(4)[-sample[motif_len]][2]
+     sample3[motif_len] <- seq(4)[-sample[motif_len]][3]
+     sample_score_r <- log(maxjointprob(sample[seq(2 * motif_len - 1)])) -
+       log(c(maxjointprob(sample1[seq(2 * motif_len - 1)]),
+             maxjointprob(sample2[seq(2 * motif_len - 1)]),
+             maxjointprob(sample3[seq(2 * motif_len - 1)])))
+     expect_equal(sample_score_r, sample_score[2:4])
+   }
+   
+   ## Use C code to generate a random sample
+   for(i in seq(10)) {
+     sample <- .Call("test_importance_sample_change", test_score, snpInfo$prior, trans_mat, test_pwm, theta, package = "atSNP")
+     start_pos <- sample[2 * motif_len] + 1
+     adj_score <- 0
+     for(s in seq_len(motif_len)) {
+       adj_s <- sum(log(adj_mat[cbind(seq(motif_len), sample[s - 1 + seq(motif_len)] + 1)]) -
+                    log(snpInfo$prior[sample[s - 1 + seq(motif_len)] + 1]))
+       adj_s <- adj_s + theta * log(test_score[motif_len + 1 - s, sample[motif_len] + 1]) -
+           log(adj_mat[motif_len + 1 - s, sample[motif_len] + 1])
+       adj_score <- adj_score + exp(adj_s)
+     }
+     sample_score <- .Call("test_compute_sample_score_change", test_pwm, test_score, adj_mat, sample[seq(2 * motif_len - 1)], snpInfo$prior, trans_mat, sample[2 * motif_len], theta, package = "atSNP")
+     expect_equal(adj_score, sample_score[1])
+   }
+ })
Test passed 
> 
> test_that("Error: compute the normalizing constant.", {
+   ## parameters
+   for(p in seq(9) / 10) {
+     delta <- .Call("test_find_percentile_change", score_diff, p, package = "atSNP")
+     theta <- .Call("test_find_theta_change", test_score, adj_mat, delta, package = "atSNP")
+     const <- .Call("test_func_delta_change", test_score, adj_mat, theta, package = "atSNP")
+     ## in R
+     adj_sum <- rowSums(adj_mat)
+     wei_sum <- rowSums(test_score ^ theta)
+     const.r <- prod(adj_sum) * sum(wei_sum / adj_sum)
+     expect_equal(const, const.r)
+   }
+ })
Test passed 
> 
> test_that("Error: sample distributions are not expected.", {
+   ## parameters
+   p <- 0.1
+   delta <- .Call("test_find_percentile_change", score_diff, p, package = "atSNP")
+   theta <- .Call("test_find_theta_change", test_score, adj_mat, delta, package = "atSNP")
+   prob_start <- rev(rowSums(test_score ^ theta) / rowSums(adj_mat))
+   ## construct the delta matrix
+   delta <- matrix(1, nrow = 4 * motif_len, ncol = 2 * motif_len - 1)
+   for(pos in seq(motif_len)) {
+     delta[seq(4) + 4 * (pos - 1), ] <- snpInfo$prior
+     delta[seq(4) + 4 * (pos - 1), pos - 1 + seq(motif_len)] <- t(test_pwm)
+     delta[seq(4) + 4 * (pos - 1), motif_len] <- test_score[motif_len + 1 - pos, ] ^ theta
+     delta[seq(4) + 4 * (pos - 1), ] <- delta[seq(4) + 4 * (pos - 1),] / rep(colSums(delta[seq(4) + 4 * (pos - 1), ]), each = 4)
+   }
+   target_freq <- matrix(0, nrow = 4, ncol = 2 * motif_len - 1)
+   for(pos in seq(motif_len)) {
+     target_freq <- target_freq + delta[seq(4) + 4 * (pos - 1), ] * prob_start[pos]
+   }
+   target_freq <- t(target_freq)
+   target_freq <- target_freq / rowSums(target_freq)
+ 
+   results_i <- function(i) {
+     ## generate 100 samples
+     sample1 <- sapply(seq(100), function(x)
+       .Call("test_importance_sample_change",
+             adj_mat, snpInfo$prior, trans_mat, test_score, theta, package = "atSNP"))
+     emp_freq1 <- get_freq(sample1)
+     sample2 <- sapply(rep(theta, 100), drawonesample)
+     emp_freq2 <- get_freq(sample2 - 1)
+     ##    print(rbind(emp_freq1[10, ], emp_freq2[10, ], target_freq[10, ]))
+     max(abs(emp_freq1 - target_freq)) > max(abs(emp_freq2 - target_freq))
+   }
+   
+   if(Sys.info()[["sysname"]] == "Windows"){
+     snow <- SnowParam(workers = 1, type = "SOCK")
+     results<-bpmapply(results_i, seq(20), BPPARAM = snow,SIMPLIFY = FALSE)
+   }else{
+     results<-bpmapply(results_i, seq(20), BPPARAM = MulticoreParam(workers = 1),
+                               SIMPLIFY = FALSE)
+   }
+ 
+   print(sum(unlist(results)))
+   print(pbinom(sum(unlist(results)), size = 20, prob = 0.5))
+ })
[1] 8
[1] 0.2517223
-- Skip (???): Error: sample distributions are not expected. -------------------
Reason: empty test

> 
> test_that("Error: the chosen pvalues should have the smaller variance.", {
+   .structure_diff <- function(pval_mat) {
+     id <- apply(pval_mat[, c(2, 4)], 1, which.min)
+     return(cbind(pval_mat[, c(1, 3)][cbind(seq_along(id), id)],
+                  pval_mat[, c(2, 4)][cbind(seq_along(id), id)]))
+   }
+   for(p in c(0.05, 0.1, 0.2, 0.5)) {
+     p_values <- .Call("test_p_value_change", test_pwm, test_score, adj_mat, snpInfo$prior, snpInfo$transition, score_diff, pval_ratio, quantile(score_diff, 1 - p), 100, package = "atSNP")$score
+     p_values_s <- .structure_diff(p_values)
+     expect_equal(p_values_s[, 2], apply(p_values[, c(2, 4)], 1, min))
+   }
+ })
Test passed 
> 
> proc.time()
   user  system elapsed 
  11.45    0.67   12.10


R Under development (unstable) (2021-11-21 r81221) -- "Unsuffered Consequences"
Copyright (C) 2021 The R Foundation for Statistical Computing
Platform: x86_64-w64-mingw32/x64 (64-bit)

R is free software and comes with ABSOLUTELY NO WARRANTY.
You are welcome to redistribute it under certain conditions.
Type 'license()' or 'licence()' for distribution details.

R is a collaborative project with many contributors.
Type 'contributors()' for more information and
'citation()' on how to cite R or R packages in publications.

Type 'demo()' for some demos, 'help()' for on-line help, or
'help.start()' for an HTML browser interface to help.
Type 'q()' to quit R.

> library(atSNP)
> library(BiocParallel)
> library(testthat)
> data(example)
> 
> trans_mat <- matrix(rep(snpInfo$prior, each = 4), nrow = 4)
> test_pwm <- motif_library$SIX5_disc1
> scores <- as.matrix(motif_scores$motif.scores[3:4, 4:5])
> score_diff <- abs(scores[,2]-scores[,1])
> 
> test_score <- test_pwm
> for(i in seq(nrow(test_score))) {
+   for(j in seq(ncol(test_score))) {
+     test_score[i, j] <- exp(mean(log(test_pwm[i, j] / test_pwm[i, -j])))
+   }
+ }
> 
> adj_mat <- test_pwm + rowMeans(test_pwm)
> motif_len <- nrow(test_pwm)
> 
> ## these are functions for this test only
> drawonesample <- function(theta) {
+     prob_start <- sapply(seq(motif_len),
+                          function(j)
+                              sum(snpInfo$prior * test_score[motif_len + 1 - j, ] ^ theta *
+                                      adj_mat[motif_len + 1 - j, ]) /
+                                          sum(snpInfo$prior * adj_mat[motif_len + 1 - j, ])
+                          )
+     id <- sample(seq(motif_len), 1, prob = prob_start)
+     sample <- sample(1:4, 2 * motif_len - 1, replace = TRUE, prob = snpInfo$prior)
+     delta <- adj_mat
+     delta[motif_len + 1 - id, ] <- delta[motif_len + 1 - id, ] * test_score[motif_len + 1 - id, ] ^ theta
+     sample[id - 1 + seq(motif_len)] <- apply(delta, 1, function(x)
+         sample(seq(4), 1, prob = x * snpInfo$prior))
+     sc <- 0
+     for(s in seq(motif_len)) {
+       delta <- adj_mat
+       delta[motif_len + 1 - s, ] <- delta[motif_len + 1 - s, ] * test_score[motif_len + 1 - s, ] ^ theta
+       sc <- sc + prod(delta[cbind(seq(motif_len), sample[s - 1 + seq(motif_len)])])
+     }
+     sample <- c(sample, id, sc)
+     return(sample)
+ }
> jointprob <- function(x) prod(test_pwm[cbind(seq(motif_len), x)])
> maxjointprob <- function(x) {
+   maxp <- -Inf
+   p <- -Inf
+   for(i in 1:motif_len) {
+     p <- jointprob(x[i:(i+motif_len - 1)])
+     if(p > maxp)
+       maxp <- p
+   }
+   for(i in 1:motif_len) {
+     p <- jointprob(5 - x[(i+motif_len - 1):i])
+     if(p > maxp)
+       maxp <- p
+   }
+   return(maxp)
+ }
> get_freq <- function(sample) {
+   emp_freq <- matrix(0, nrow = 2 * motif_len - 1, ncol = 4)
+   for(i in seq(2 * motif_len - 1)) {
+     for(j in seq(4)) {
+       emp_freq[i, j] <- sum(sample[i, ] == j - 1)
+     }
+   }
+   emp_freq <- emp_freq / rowSums(emp_freq)
+   return(emp_freq)
+ }
> 
> test_that("Error: quantile function computing are not equivalent.", {
+   for(p in c(0.01, 0.1, 0.5, 0.9, 0.99)) {
+     delta <- .Call("test_find_percentile_diff", score_diff, p, package = "atSNP")
+     delta.r <- as.double(sort(abs(scores[,2]-scores[,1]))[ceiling((1 - p) * (nrow(scores)))])
+     expect_equal(delta, delta.r)
+   }
+ })
Test passed 
> 
> test_that("Error: the scores for samples are not equivalent.", {
+   p <- 0.1
+   delta <- .Call("test_find_percentile_diff", score_diff, p, package = "atSNP")
+   theta <- .Call("test_find_theta_diff", test_score, adj_mat, snpInfo$prior, snpInfo$transition, delta, package = "atSNP")
+   ## Use R code to generate a random sample
+   for(i in seq(10)) {
+     sample <- drawonesample(theta)
+     sample_score <- .Call("test_compute_sample_score_diff", test_pwm, test_score, adj_mat, sample[seq(2 * motif_len - 1)] - 1, sample[2 * motif_len] - 1, theta, package = "atSNP")
+     expect_equal(sample[2 * motif_len + 1], sample_score[1])
+     sample1 <- sample2 <- sample3 <- sample
+     sample1[motif_len] <- seq(4)[-sample[motif_len]][1]
+     sample2[motif_len] <- seq(4)[-sample[motif_len]][2]
+     sample3[motif_len] <- seq(4)[-sample[motif_len]][3]
+     sample_score_r <- log(maxjointprob(sample[seq(2 * motif_len - 1)])) -
+       log(c(maxjointprob(sample1[seq(2 * motif_len - 1)]),
+             maxjointprob(sample2[seq(2 * motif_len - 1)]),
+             maxjointprob(sample3[seq(2 * motif_len - 1)])))
+     expect_equal(sample_score_r, sample_score[-1])
+   }
+   
+   ## Use C code to generate a random sample
+   delta <- matrix(1, nrow = 4 * motif_len, ncol = 2 * motif_len - 1)
+   for(pos in seq(motif_len)) {
+       for(j in (pos + motif_len - 1) : 1) {
+           if(j < pos + motif_len - 1) {
+               delta[4 * (pos - 1) + seq(4), j] <- sum(snpInfo$prior * delta[4 * (pos - 1) + seq(4), j + 1])
+           }
+           if(j >= pos) {
+               delta[4 * (pos - 1) + seq(4), j] <- delta[4 * (pos - 1) + seq(4), j] * adj_mat[j - pos + 1, ]
+           }
+           if(j == motif_len) {
+               delta[4 * (pos - 1) + seq(4), j] <- delta[4 * (pos - 1) + seq(4), j] * test_score[j - pos + 1, ] ^ theta
+           }
+       }
+   }
+   for(i in seq(10)) {
+     sample <- .Call("test_importance_sample_diff", delta, snpInfo$prior, trans_mat, test_pwm, theta, package = "atSNP")
+     start_pos <- sample[2 * motif_len] + 1
+     adj_score <- 0
+     for(s in seq_len(motif_len)) {
+       adj_s <- sum(log(adj_mat[cbind(seq(motif_len), sample[s - 1 + seq(motif_len)] + 1)]))
+       adj_s <- adj_s + theta * log(test_score[motif_len + 1 - s, sample[motif_len] + 1])
+       adj_score <- adj_score + exp(adj_s)
+     }
+     sample_score <- .Call("test_compute_sample_score_diff", test_pwm, test_score, adj_mat, sample[seq(2 * motif_len - 1)], sample[2 * motif_len], theta, package = "atSNP")
+     expect_equal(adj_score, sample_score[1])
+   }
+ })
Test passed 
> 
> test_that("Error: compute the normalizing constant.", {
+ 
+   ## parameters
+   p <- 0.1
+   delta <- .Call("test_find_percentile_diff", score_diff, p, package = "atSNP")
+   theta <- .Call("test_find_theta_diff", test_score, adj_mat, snpInfo$prior, snpInfo$transition, delta, package = "atSNP")
+   
+   ##
+   const <- .Call("test_func_delta_diff", test_score, adj_mat, snpInfo$prior, trans_mat, theta, package = "atSNP")
+ 
+    prob_start <- sapply(seq(motif_len),
+                          function(j)
+                              sum(snpInfo$prior * test_score[motif_len + 1 - j, ] ^ theta *
+                                      adj_mat[motif_len + 1 - j, ]) /
+                                          sum(snpInfo$prior * adj_mat[motif_len + 1 - j, ])
+                          )
+   
+   const.r <- prod(colSums(snpInfo$prior * t(adj_mat))) * sum(prob_start)
+   expect_equal(const, const.r)
+ })
Test passed 
> 
> test_that("Error: sample distributions are not expected.", {
+   
+   ## parameters
+   p <- 0.1
+   delta <- .Call("test_find_percentile_diff", score_diff, p, package = "atSNP")
+   theta <- .Call("test_find_theta_diff", test_score, adj_mat, snpInfo$prior, snpInfo$transition, delta, package = "atSNP")
+ 
+   ## construct the delta matrix
+   delta <- matrix(1, nrow = 4 * motif_len, ncol = 2 * motif_len - 1)
+    for(pos in seq(motif_len)) {
+         for(j in (pos + motif_len - 1) : 1) {
+             if(j < pos + motif_len - 1) {
+                 delta[4 * (pos - 1) + seq(4), j] <- sum(snpInfo$prior * delta[4 * (pos - 1) + seq(4), j + 1])
+             }
+             if(j >= pos) {
+                 delta[4 * (pos - 1) + seq(4), j] <- delta[4 * (pos - 1) + seq(4), j] * adj_mat[j - pos + 1, ]
+             }
+             if(j == motif_len) {
+                 delta[4 * (pos - 1) + seq(4), j] <- delta[4 * (pos - 1) + seq(4), j] * test_score[j - pos + 1, ] ^ theta
+             }
+         }
+     }
+ 
+   target_freq <- matrix(0, nrow = 4, ncol = 2 * motif_len - 1)
+   
+   mat <- snpInfo$prior * matrix(delta[, 1], nrow = 4)
+   wei <- colSums(mat)
+   for(j in seq(2 * motif_len - 1)) {
+       for(pos in seq(motif_len)) {
+           tmp <- delta[seq(4) + 4 * (pos - 1), j] * snpInfo$prior
+           target_freq[, j] <- target_freq[, j] +  tmp / sum(tmp) * wei[pos]
+       }
+   }
+   target_freq <- t(target_freq)
+   target_freq <- target_freq / rowSums(target_freq)
+ 
+   results_i <- function(i) {
+     ## generate 100 samples
+     sample1 <- sapply(seq(100), function(x)
+       .Call("test_importance_sample_diff",
+             delta, snpInfo$prior, trans_mat, test_score, theta, package = "atSNP"))
+     emp_freq1 <- get_freq(sample1)
+     
+     sample2 <- sapply(rep(theta, 100), drawonesample)
+     emp_freq2 <- get_freq(sample2 - 1)
+     
+     ##    print(rbind(emp_freq1[10, ], emp_freq2[10, ], target_freq[10, ]))
+     max(abs(emp_freq1 - target_freq)) > max(abs(emp_freq2 - target_freq))
+   }
+  
+   if(Sys.info()[["sysname"]] == "Windows"){
+     snow <- SnowParam(workers = 1, type = "SOCK")
+     results<-bpmapply(results_i, seq(20), BPPARAM = snow,SIMPLIFY = FALSE)
+   }else{
+     results<-bpmapply(results_i, seq(20), BPPARAM = MulticoreParam(workers = 1),
+                       SIMPLIFY = FALSE)
+   }
+   
+   print(sum(unlist(results)))
+ 
+   print(pbinom(sum(unlist(results)), size = 20, prob = 0.5))
+   
+ })
[1] 12
[1] 0.868412
-- Skip (???): Error: sample distributions are not expected. -------------------
Reason: empty test

> 
> test_that("Error: the chosen pvalues should have the smaller variance.", {
+ 
+   .structure_diff <- function(pval_mat) {
+     id <- apply(pval_mat[, c(2, 4)], 1, which.min)
+     return(cbind(pval_mat[, c(1, 3)][cbind(seq_along(id), id)],
+                  pval_mat[, c(2, 4)][cbind(seq_along(id), id)]))
+   }
+   
+   for(p in c(0.05, 0.1, 0.2, 0.5)) {
+     p_values <- .Call("test_p_value_diff", test_pwm, test_score, adj_mat, snpInfo$prior, snpInfo$transition, score_diff, quantile(score_diff, 1 - p), 100, package = "atSNP")
+     p_values_s <- .structure_diff(p_values)
+     expect_equal(p_values_s[, 2], apply(p_values[, c(2, 4)], 1, min))
+   }
+ })
Test passed 
> 
> proc.time()
   user  system elapsed 
  11.23    0.64   11.84


R Under development (unstable) (2021-11-21 r81221) -- "Unsuffered Consequences"
Copyright (C) 2021 The R Foundation for Statistical Computing
Platform: x86_64-w64-mingw32/x64 (64-bit)

R is free software and comes with ABSOLUTELY NO WARRANTY.
You are welcome to redistribute it under certain conditions.
Type 'license()' or 'licence()' for distribution details.

R is a collaborative project with many contributors.
Type 'contributors()' for more information and
'citation()' on how to cite R or R packages in publications.

Type 'demo()' for some demos, 'help()' for on-line help, or
'help.start()' for an HTML browser interface to help.
Type 'q()' to quit R.

> library(atSNP)
> library(BiocParallel)
> library(testthat)
> data(example)
> 
> trans_mat <- matrix(rep(snpInfo$prior, each = 4), nrow = 4)
> test_pwm <- motif_library$SIX5_disc1
> scores <- as.matrix(motif_scores$motif.scores[3:4, 4:5])
> 
> motif_len <- nrow(test_pwm)
> 
> ## these are functions for this test only
> drawonesample <- function(theta) {
+   delta <- snpInfo$prior * t(test_pwm ^ theta)
+   delta <- delta / rep(colSums(delta), each = 4)
+   sample <- sample(1:4, 2 * motif_len - 1, replace = TRUE, prob = snpInfo$prior)
+   id <- sample(seq(motif_len), 1)
+   sample[id : (id + motif_len - 1)] <- apply(delta, 2, function(x) sample(1:4, 1, prob = x))
+   sc <- s_cond <- 0
+   for(s in seq(motif_len)) {
+     sc <- sc + prod(test_pwm[cbind(seq(motif_len),
+                                   sample[s : (s + motif_len - 1)])]) ^ theta
+   }
+   s_cond <- prod(test_pwm[cbind(seq(motif_len),
+                                 sample[id : (id + motif_len - 1)])]) ^ theta
+   sample <- c(sample, id, sc, s_cond)
+   return(sample)
+ }
> jointprob <- function(x) prod(test_pwm[cbind(seq(motif_len), x)])
> maxjointprob <- function(x) {
+   maxp <- -Inf
+   p <- -Inf
+   for(i in 1:motif_len) {
+     p <- jointprob(x[i:(i+motif_len - 1)])
+     if(p > maxp)
+       maxp <- p
+   }
+   for(i in 1:motif_len) {
+     p <- jointprob(5 - x[(i+motif_len - 1):i])
+     if(p > maxp)
+       maxp <- p
+   }
+   return(maxp)
+ }
> get_freq <- function(sample) {
+   ids <- cbind(
+                rep(sample[motif_len * 2, ], each = motif_len) + seq(motif_len),
+                rep(seq(100), each = motif_len))
+   sample_motif <- matrix(sample[ids], nrow = motif_len) + 1
+   emp_freq <- matrix(0, nrow = motif_len, ncol = 4)
+   for(i in seq(motif_len)) {
+     for(j in seq(4)) {
+       emp_freq[i, j] <- sum(sample_motif[i, ] == j)
+     }
+   }
+   emp_freq <- emp_freq / rowSums(emp_freq)
+   return(emp_freq)
+ }
> 
> test_that("Error: quantile function computing are not equivalent.", {
+   for(p in c(0.01, 0.1, 0.5, 0.9, 0.99)) {
+     delta <- .Call("test_find_percentile", c(scores), p, package = "atSNP")
+     delta.r <- -sort(-c(scores))[as.integer(p * length(scores)) + 1]
+     expect_equal(delta, delta.r)
+   }
+ })
Test passed 
> 
> test_that("Error: the scores for samples are not equivalent.", {
+   p <- 0.01
+   delta <- .Call("test_find_percentile", scores, p, package = "atSNP")
+   theta <- .Call("test_find_theta", test_pwm, snpInfo$prior, snpInfo$transition, delta, package = "atSNP")
+   ## Use R code to generate a random sample
+   for(i in seq(10)) {
+     sample <- drawonesample(theta)
+     sample_score <- .Call("test_compute_sample_score", test_pwm, sample[seq(2 * motif_len - 1)] - 1, sample[motif_len * 2] - 1, theta, package = "atSNP")
+     expect_equal(sample[2 * motif_len + 1], sample_score[2])
+     expect_equal(sample[2 * motif_len + 2], sample_score[3])
+   }
+   ## Use C code to generate a random sample
+   for(i in seq(10)) {
+     delta <- t(test_pwm ^ theta)
+     delta <- cbind(matrix(
+                           sum(snpInfo$prior * delta[, 1]),
+                           nrow = 4, ncol = motif_len - 1), delta)
+     sample <- .Call("test_importance_sample", delta, snpInfo$prior, trans_mat, test_pwm, theta, package = "atSNP")
+     start_pos <- sample[motif_len * 2]
+     adj_score <- 0
+     for(s in seq(motif_len) - 1) {
+       adj_score <- adj_score + prod(test_pwm[cbind(seq(motif_len),
+                                                    sample[s + seq(motif_len)] + 1)]) ^ theta
+     }
+     adj_score_cond <- prod(test_pwm[cbind(seq(motif_len), sample[start_pos + seq(motif_len)] + 1)]) ^ theta
+     sample_score <- .Call("test_compute_sample_score", test_pwm, sample[seq(2 * motif_len - 1)], sample[motif_len * 2], theta, package = "atSNP")
+     expect_equal(adj_score, sample_score[2])
+     expect_equal(adj_score_cond, sample_score[3])
+   }
+ })
Test passed 
> 
> test_that("Error: compute the normalizing constant.", {
+   ## parameters
+   p <- 0.01
+   delta <- .Call("test_find_percentile", scores, p, package = "atSNP")
+   theta <- .Call("test_find_theta", test_pwm, snpInfo$prior, snpInfo$transition, delta, package = "atSNP")
+   ##
+   const <- .Call("test_func_delta", test_pwm, snpInfo$prior, trans_mat, theta, package = "atSNP")
+   const.r <- prod(colSums(snpInfo$prior * t(test_pwm) ^ theta)) * motif_len
+   expect_equal(abs(const - const.r) / const < 1e-5, TRUE)
+ })
Test passed 
> 
> test_that("Error: sample distributions are not expected.", {
+   ## parameters
+   p <- 0.1
+   delta <- .Call("test_find_percentile", scores, p, package = "atSNP")
+   theta <- .Call("test_find_theta", test_pwm, snpInfo$prior, trans_mat, delta, package = "atSNP")
+   delta <- t(test_pwm ^ theta)
+   delta <- cbind(matrix(
+                         sum(snpInfo$prior * delta[, 1]),
+                         nrow = 4, ncol = motif_len - 1), delta)
+ 
+   results_i <- function(i) {
+     ## generate 100 samples
+     sample <- sapply(seq(100), function(x)
+                      .Call("test_importance_sample",
+                            delta, snpInfo$prior, trans_mat, test_pwm, theta, package = "atSNP"))
+     emp_freq1 <- get_freq(sample)
+     target_freq <- test_pwm ^ theta * snpInfo$prior
+     target_freq <- target_freq / rowSums(target_freq)
+     ## generate samples in R
+     sample <- sapply(rep(theta, 100), drawonesample)
+     emp_freq2 <- get_freq(sample[seq(2 * motif_len), ] - 1)
+     max(abs(emp_freq1 - target_freq)) > max(abs(emp_freq2 - target_freq))
+   }
+ 
+   if(Sys.info()[["sysname"]] == "Windows"){
+     snow <- SnowParam(workers = 1, type = "SOCK")
+     results<-bpmapply(results_i, seq(20), BPPARAM = snow,SIMPLIFY = FALSE)
+   }else{
+     results<-bpmapply(results_i, seq(20), BPPARAM = MulticoreParam(workers = 1),
+                       SIMPLIFY = FALSE)
+   }
+   
+   print(sum(unlist(results)))
+   print(pbinom(sum(unlist(results)), size = 20, prob = 0.5))
+ })
[1] 7
[1] 0.131588
-- Skip (???): Error: sample distributions are not expected. -------------------
Reason: empty test

> 
> test_that("Error: the chosen pvalues should have the smaller variance.", {
+   .structure <- function(pval_mat) {
+     id1 <- apply(pval_mat[, c(2, 4)], 1, which.min)
+     return(cbind(
+                  pval_mat[, c(1, 3)][cbind(seq_along(id1), id1)],
+                  pval_mat[, c(2, 4)][cbind(seq_along(id1), id1)])
+            )
+   }
+   for(p in c(0.01, 0.05, 0.1)) {
+     theta <- .Call("test_find_theta", test_pwm, snpInfo$prior, trans_mat, quantile(c(scores), 1 - p), package = "atSNP")
+     p_values <- .Call("test_p_value", test_pwm, snpInfo$prior, snpInfo$transition, c(scores), theta, 100, package = "atSNP")
+     p_values_s <- .structure(p_values)
+     expect_equal(p_values_s[, 2], apply(p_values[, c(2, 4)], 1, min))
+   }
+ })
Test passed 
> 
> proc.time()
   user  system elapsed 
  10.54    0.62   11.14

CHECK results for atSNP on riesling1

Summary

Command output

Installation output

Tests output

Example timings

name	user	system	elapsed
ComputeMotifScore	0.80	0.03	10.72
ComputePValues	0.75	0.03	12.56
GetIUPACSequence	0	0	0
LoadFastaData	0.17	0.03	0.21
LoadMotifLibrary	0.14	0.02	0.17
LoadSNPData	0	0	0
MatchSubsequence	0.62	0.00	10.70
dtMotifMatch	0.68	0.00	11.63
plotMotifMatch	0.78	0.03	0.84