Back to Multiple platform build/check report for BioC 3.14 |
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This page was generated on 2022-04-13 12:07:19 -0400 (Wed, 13 Apr 2022).
Hostname | OS | Arch (*) | R version | Installed pkgs |
---|---|---|---|---|
nebbiolo2 | Linux (Ubuntu 20.04.4 LTS) | x86_64 | 4.1.3 (2022-03-10) -- "One Push-Up" | 4324 |
tokay2 | Windows Server 2012 R2 Standard | x64 | 4.1.3 (2022-03-10) -- "One Push-Up" | 4077 |
machv2 | macOS 10.14.6 Mojave | x86_64 | 4.1.3 (2022-03-10) -- "One Push-Up" | 4137 |
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 |
To the developers/maintainers of the scMerge package: - Please allow up to 24 hours (and sometimes 48 hours) for your latest push to git@git.bioconductor.org:packages/scMerge.git to reflect on this report. See How and When does the builder pull? When will my changes propagate? for more information. - Make sure to use the following settings in order to reproduce any error or warning you see on this page. |
Package 1730/2083 | Hostname | OS / Arch | INSTALL | BUILD | CHECK | BUILD BIN | ||||||||
scMerge 1.10.0 (landing page) Yingxin Lin
| nebbiolo2 | Linux (Ubuntu 20.04.4 LTS) / x86_64 | OK | OK | OK | |||||||||
tokay2 | Windows Server 2012 R2 Standard / x64 | OK | OK | OK | OK | |||||||||
machv2 | macOS 10.14.6 Mojave / x86_64 | OK | OK | OK | OK | |||||||||
Package: scMerge |
Version: 1.10.0 |
Command: C:\Users\biocbuild\bbs-3.14-bioc\R\bin\R.exe CMD check --force-multiarch --install=check:scMerge.install-out.txt --library=C:\Users\biocbuild\bbs-3.14-bioc\R\library --no-vignettes --timings scMerge_1.10.0.tar.gz |
StartedAt: 2022-04-13 02:27:11 -0400 (Wed, 13 Apr 2022) |
EndedAt: 2022-04-13 02:33:50 -0400 (Wed, 13 Apr 2022) |
EllapsedTime: 399.4 seconds |
RetCode: 0 |
Status: OK |
CheckDir: scMerge.Rcheck |
Warnings: 0 |
############################################################################## ############################################################################## ### ### Running command: ### ### C:\Users\biocbuild\bbs-3.14-bioc\R\bin\R.exe CMD check --force-multiarch --install=check:scMerge.install-out.txt --library=C:\Users\biocbuild\bbs-3.14-bioc\R\library --no-vignettes --timings scMerge_1.10.0.tar.gz ### ############################################################################## ############################################################################## * using log directory 'C:/Users/biocbuild/bbs-3.14-bioc/meat/scMerge.Rcheck' * using R version 4.1.3 (2022-03-10) * using platform: x86_64-w64-mingw32 (64-bit) * using session charset: ISO8859-1 * using option '--no-vignettes' * checking for file 'scMerge/DESCRIPTION' ... OK * checking extension type ... Package * this is package 'scMerge' version '1.10.0' * package encoding: UTF-8 * 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 'scMerge' 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 * loading checks for arch 'i386' ** 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 * loading checks for arch 'x64' ** 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 Namespace in Imports field not imported from: 'parallel' 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 ... OK * 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 files in 'vignettes' ... OK * checking examples ... ** running examples for arch 'i386' ... OK ** running examples for arch 'x64' ... OK * checking for unstated dependencies in 'tests' ... OK * checking tests ... ** running tests for arch 'i386' ... Running 'testthat.R' OK ** running tests for arch 'x64' ... Running 'testthat.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: 1 NOTE See 'C:/Users/biocbuild/bbs-3.14-bioc/meat/scMerge.Rcheck/00check.log' for details.
scMerge.Rcheck/00install.out
############################################################################## ############################################################################## ### ### Running command: ### ### C:\cygwin\bin\curl.exe -O http://155.52.207.166/BBS/3.14/bioc/src/contrib/scMerge_1.10.0.tar.gz && rm -rf scMerge.buildbin-libdir && mkdir scMerge.buildbin-libdir && C:\Users\biocbuild\bbs-3.14-bioc\R\bin\R.exe CMD INSTALL --merge-multiarch --build --library=scMerge.buildbin-libdir scMerge_1.10.0.tar.gz && C:\Users\biocbuild\bbs-3.14-bioc\R\bin\R.exe CMD INSTALL scMerge_1.10.0.zip && rm scMerge_1.10.0.tar.gz scMerge_1.10.0.zip ### ############################################################################## ############################################################################## % Total % Received % Xferd Average Speed Time Time Time Current Dload Upload Total Spent Left Speed 0 0 0 0 0 0 0 0 --:--:-- --:--:-- --:--:-- 0 15 3369k 15 529k 0 0 748k 0 0:00:04 --:--:-- 0:00:04 748k 63 3369k 63 2148k 0 0 1262k 0 0:00:02 0:00:01 0:00:01 1262k 100 3369k 100 3369k 0 0 1516k 0 0:00:02 0:00:02 --:--:-- 1517k install for i386 * installing *source* package 'scMerge' ... ** using staged installation ** R ** data ** inst ** byte-compile and prepare package for lazy loading ** help *** installing help indices converting help for package 'scMerge' finding HTML links ... done example_sce html fastRUVIII html ruvSimulate html scMerge html scRUVIII html scRUVg html scReplicate html scSEGIndex html sce_cbind html segList html segList_ensemblGeneID 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 install for x64 * installing *source* package 'scMerge' ... ** testing if installed package can be loaded * MD5 sums packaged installation of 'scMerge' as scMerge_1.10.0.zip * DONE (scMerge) * installing to library 'C:/Users/biocbuild/bbs-3.14-bioc/R/library' package 'scMerge' successfully unpacked and MD5 sums checked
scMerge.Rcheck/tests_i386/testthat.Rout R version 4.1.3 (2022-03-10) -- "One Push-Up" Copyright (C) 2022 The R Foundation for Statistical Computing Platform: i386-w64-mingw32/i386 (32-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(testthat) > library(scMerge) > > test_check("scMerge") Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 4 Dimension of the replicates mapping matrix: [1] 200 3 Selecting optimal RUVk Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 3 2 1 5 2 2 2 6 1 2 3 Dimension of the replicates mapping matrix: [1] 200 3 Could not find a batch column in colData(sce_combine)Selecting optimal RUVk No cell type info, replicate matrix will be used as cell type info Performing supervised scMerge with: 1. Cell type information 2. No cell type indices 3. No mutual nearest neighbour clustering Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 3 2 1 5 2 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 4. No supplied marker but supplied marker_list for MNN clustering Taking the union of marker_list as the markers 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. Cell type indices 3. No mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 1 1 2 3 2 1 3 4 3 2 1 5 2 2 2 6 1 2 3 7. Finishing semi-supervised scMerge with subsets of known cell type Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 1 2 1 5 3 2 2 6 2 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker but supplied marker_list for MNN clustering Taking the union of marker_list as the markers 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 5 4 2 2 6 5 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 1 2 1 5 3 2 2 6 2 2 3 7. Performing semi-supervised scMerge with wanted variation Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 1 1 2 3 2 1 3 4 3 2 1 5 2 2 2 6 1 2 3 7. Performing semi-supervised scMerge with wanted variation Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 36 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 36 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 1 1 2 3 3 1 3 4 1 2 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 63 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 5 2 2 2 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 63 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 2 2 1 5 1 2 2 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 24 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 1 1 1 2 2 2 1 3 1 3 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 24 HVG were found 5. 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|======================================================================| 100% [ FAIL 0 | WARN 0 | SKIP 0 | PASS 36 ] > > proc.time() user system elapsed 37.15 2.46 39.64 |
scMerge.Rcheck/tests_x64/testthat.Rout R version 4.1.3 (2022-03-10) -- "One Push-Up" Copyright (C) 2022 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(testthat) > library(scMerge) > > test_check("scMerge") Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 100 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 3 Dimension of the replicates mapping matrix: [1] 200 4 Dimension of the replicates mapping matrix: [1] 200 3 Selecting optimal RUVk Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 3 2 1 5 2 2 2 6 1 2 3 Dimension of the replicates mapping matrix: [1] 200 3 Could not find a batch column in colData(sce_combine)Selecting optimal RUVk No cell type info, replicate matrix will be used as cell type info Performing supervised scMerge with: 1. Cell type information 2. No cell type indices 3. No mutual nearest neighbour clustering Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 3 2 1 5 2 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 4. No supplied marker but supplied marker_list for MNN clustering Taking the union of marker_list as the markers 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. No cell type indices 3. Mutual nearest neighbour clustering 5. Calculating supervised clustering list 6. Create Mutual Nearest Clusters. Preview cells-to-cell_type matching graph and matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing semi-supervised scMerge with: 1. Cell type information 2. Cell type indices 3. No mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 1 1 2 3 2 1 3 4 3 2 1 5 2 2 2 6 1 2 3 7. Finishing semi-supervised scMerge with subsets of known cell type Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 1 2 1 5 3 2 2 6 2 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker but supplied marker_list for MNN clustering Taking the union of marker_list as the markers 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 5 4 2 2 6 5 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 4 2 1 5 5 2 2 6 1 2 3 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 1 2 1 5 3 2 2 6 2 2 3 7. Performing semi-supervised scMerge with wanted variation Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 75 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 1 1 2 3 2 1 3 4 3 2 1 5 2 2 2 6 1 2 3 7. Performing semi-supervised scMerge with wanted variation Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 36 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 36 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 1 1 2 3 3 1 3 4 1 2 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 63 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 2 1 1 2 3 1 2 3 1 1 3 4 1 2 1 5 2 2 2 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 63 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 3 1 1 2 2 1 2 3 1 1 3 4 2 2 1 5 1 2 2 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 24 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. Preview cells-cell_type matching output matrix: group batch cluster 1 1 1 1 2 2 2 1 3 1 3 1 Performing unsupervised scMerge with: 1. No cell type information 2. Cell type indices not relevant here 3. Mutual nearest neighbour matching 4. No supplied marker and no supplied marker_list for MNN clustering Finding Highly Variable Genes for clustering 24 HVG were found 5. PCA and Kmeans clustering will be performed on each batch 6. Create Mutual Nearest Clusters. 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|======================================================================| 100% [ FAIL 0 | WARN 0 | SKIP 0 | PASS 36 ] > > proc.time() user system elapsed 42.06 1.21 43.29 |
scMerge.Rcheck/examples_i386/scMerge-Ex.timings
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scMerge.Rcheck/examples_x64/scMerge-Ex.timings
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