Stefano Mangiola
| Snapshot Date: 2024-05-01 14:05:06 -0400 (Wed, 01 May 2024) |
| git_url: https://git.bioconductor.org/packages/tidybulk |
| git_branch: devel |
| git_last_commit: 0c757df |
| git_last_commit_date: 2024-04-30 11:21:35 -0400 (Tue, 30 Apr 2024) |
| Back to Multiple platform build/check report for BioC 3.20: simplified long |
|
This page was generated on 2024-05-03 11:38:57 -0400 (Fri, 03 May 2024).
| Hostname | OS | Arch (*) | R version | Installed pkgs |
|---|---|---|---|---|
| nebbiolo2 | Linux (Ubuntu 22.04.3 LTS) | x86_64 | 4.4.0 RC (2024-04-16 r86468) -- "Puppy Cup" | 4660 |
| palomino4 | Windows Server 2022 Datacenter | x64 | 4.4.0 RC (2024-04-16 r86468 ucrt) -- "Puppy Cup" | 4391 |
| merida1 | macOS 12.7.4 Monterey | x86_64 | 4.4.0 Patched (2024-04-24 r86482) -- "Puppy Cup" | 4422 |
| 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 | ||||
| Package 2087/2230 | Hostname | OS / Arch | INSTALL | BUILD | CHECK | BUILD BIN | ||||||||
| tidybulk 1.17.0 (landing page) Stefano Mangiola
| nebbiolo2 | Linux (Ubuntu 22.04.3 LTS) / x86_64 | OK | OK | OK | | ||||||||
| palomino4 | Windows Server 2022 Datacenter / x64 | OK | OK | OK | OK | | ||||||||
| merida1 | macOS 12.7.4 Monterey / x86_64 | OK | OK | OK | OK | | ||||||||
| kjohnson1 | macOS 13.6.6 Ventura / arm64 | see weekly results here | ||||||||||||
|
To the developers/maintainers of the tidybulk package: - Allow up to 24 hours (and sometimes 48 hours) for your latest push to git@git.bioconductor.org:packages/tidybulk.git to reflect on this report. See Troubleshooting Build Report for more information. - Use the following Renviron settings to reproduce errors and warnings. - If 'R CMD check' started to fail recently on the Linux builder(s) over a missing dependency, add the missing dependency to 'Suggests:' in your DESCRIPTION file. See Renviron.bioc for more information. |
| Package: tidybulk |
| Version: 1.17.0 |
| Command: /Library/Frameworks/R.framework/Resources/bin/R CMD check --install=check:tidybulk.install-out.txt --library=/Library/Frameworks/R.framework/Resources/library --no-vignettes --timings tidybulk_1.17.0.tar.gz |
| StartedAt: 2024-05-02 12:45:11 -0400 (Thu, 02 May 2024) |
| EndedAt: 2024-05-02 13:04:38 -0400 (Thu, 02 May 2024) |
| EllapsedTime: 1167.0 seconds |
| RetCode: 0 |
| Status: OK |
| CheckDir: tidybulk.Rcheck |
| Warnings: 0 |
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### Running command:
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### /Library/Frameworks/R.framework/Resources/bin/R CMD check --install=check:tidybulk.install-out.txt --library=/Library/Frameworks/R.framework/Resources/library --no-vignettes --timings tidybulk_1.17.0.tar.gz
###
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* using log directory ‘/Users/biocbuild/bbs-3.20-bioc/meat/tidybulk.Rcheck’
* using R version 4.4.0 Patched (2024-04-24 r86482)
* using platform: x86_64-apple-darwin20
* R was compiled by
Apple clang version 14.0.0 (clang-1400.0.29.202)
GNU Fortran (GCC) 12.2.0
* running under: macOS Monterey 12.7.4
* using session charset: UTF-8
* using option ‘--no-vignettes’
* checking for file ‘tidybulk/DESCRIPTION’ ... OK
* checking extension type ... Package
* this is package ‘tidybulk’ version ‘1.17.0’
* 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 for sufficient/correct file permissions ... OK
* checking whether package ‘tidybulk’ 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 code 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 whether startup messages can be suppressed ... OK
* checking dependencies in R code ... OK
* checking S3 generic/method consistency ... OK
* checking replacement functions ... OK
* checking foreign function calls ... OK
* checking R code for possible problems ... NOTE
.adjust_abundance_se: no visible binding for global variable ‘x’
.aggregate_duplicates_se: no visible binding for global variable
‘group_name’
.aggregate_duplicates_se: no visible binding for global variable
‘group’
.deconvolve_cellularity_se: no visible binding for global variable
‘X_cibersort’
.describe_transcript_SE: no visible binding for global variable
‘transcript’
.describe_transcript_SE: no visible binding for global variable
‘description’
.identify_abundant: no visible binding for global variable ‘.abundant’
.keep_abundant: no visible binding for global variable ‘.abundant’
.pivot_sample: no visible binding for global variable ‘.’
.quantile_normalise_abundance: no visible binding for global variable
‘x’
.quantile_normalise_abundance_se: no visible binding for global
variable ‘x’
.scale_abundance: no visible binding for global variable ‘x’
.scale_abundance: no visible binding for global variable ‘multiplier’
.scale_abundance_se: no visible binding for global variable ‘x’
.test_differential_abundance_se: no visible binding for global variable
‘.contrasts’
.test_differential_abundance_se: no visible binding for global variable
‘action’
.test_differential_cellularity: no visible binding for global variable
‘X_cibersort’
.test_differential_cellularity_se: no visible binding for global
variable ‘X_cibersort’
.test_differential_cellularity_se: no visible binding for global
variable ‘cell_type’
.test_differential_cellularity_se: no visible binding for global
variable ‘prop’
.test_differential_cellularity_se: no visible binding for global
variable ‘.cell_type’
.test_gene_enrichment_SE: no visible global function definition for
‘buildCustomIdx’
.test_gene_enrichment_SE: no visible global function definition for
‘buildIdx’
.test_gene_enrichment_SE: no visible global function definition for
‘egsea’
.test_gene_enrichment_SE: no visible binding for global variable
‘pathway’
.test_gene_enrichment_SE: no visible binding for global variable
‘data_base’
.test_gene_enrichment_SE: no visible binding for global variable
‘web_page’
.test_gene_overrepresentation: no visible binding for global variable
‘my_do_test’
.test_gene_overrepresentation_SE: no visible binding for global
variable ‘my_do_test’
.test_gene_rank: no visible global function definition for
‘with_groups’
.test_gene_rank: no visible global function definition for ‘desc’
.test_gene_rank_SE: no visible global function definition for ‘desc’
.test_stratification_cellularity: no visible binding for global
variable ‘X_cibersort’
.test_stratification_cellularity_SE: no visible binding for global
variable ‘X_cibersort’
.test_stratification_cellularity_SE: no visible binding for global
variable ‘.cell_type’
add_scaled_counts_bulk.calcNormFactor: no visible binding for global
variable ‘transcript’
aggregate_duplicated_transcripts_DT: no visible binding for global
variable ‘.abundance_scaled’
aggregate_duplicated_transcripts_bulk: no visible binding for global
variable ‘.abundance_scaled’
aggregate_duplicated_transcripts_bulk: no visible binding for global
variable ‘n_aggr’
aggregate_duplicated_transcripts_bulk: no visible global function
definition for ‘where’
as_matrix: no visible binding for global variable ‘variable’
call_core: no visible binding for global variable ‘nulldist’
change_reserved_column_names: no visible binding for global variable
‘.’
check_if_duplicated_genes: no visible binding for global variable
‘transcript’
check_if_duplicated_genes: no visible binding for global variable ‘read
count’
counts_scaled_exist_SE: no visible binding for global variable
‘tt_columns’
counts_scaled_exist_SE: no visible binding for global variable ‘.’
create_tt_from_bam_sam_bulk: no visible binding for global variable ‘.’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘temp’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘Status’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘counts’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘GeneID’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘genes’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘samples’
create_tt_from_bam_sam_bulk: no visible binding for global variable
‘transcript’
eliminate_sparse_transcripts: no visible global function definition for
‘add_count’
eliminate_sparse_transcripts: no visible binding for global variable
‘my_n’
entrez_over_to_gsea: no visible binding for global variable ‘gs_cat’
entrez_over_to_gsea: no visible binding for global variable ‘test’
entrez_over_to_gsea: no visible binding for global variable ‘geneID’
entrez_rank_to_gsea: no visible binding for global variable ‘gs_cat’
entrez_rank_to_gsea: no visible binding for global variable ‘.’
entrez_rank_to_gsea: no visible binding for global variable
‘entrez_gene’
entrez_rank_to_gsea: no visible binding for global variable ‘fit’
error_if_duplicated_genes: no visible binding for global variable
‘transcript’
error_if_duplicated_genes: no visible binding for global variable ‘read
count’
error_if_duplicated_genes: no visible global function definition for
‘desc’
error_if_log_transformed: no visible binding for global variable ‘m’
fill_NA_matrix_with_factor_colwise: no visible binding for global
variable ‘.’
fill_NA_using_formula: no visible binding for global variable ‘NUL’
fill_NA_using_formula: no visible binding for global variable ‘ct_data’
fill_NA_using_formula: no visible binding for global variable
‘library_size__’
fill_NA_using_formula: no visible binding for global variable
‘cov_data’
filter_genes_on_condition: no visible binding for global variable
‘.feature’
get_abundance_norm_if_exists: no visible binding for global variable
‘.abundance_scaled’
get_adjusted_counts_for_unwanted_variation_bulk: no visible binding for
global variable ‘.’
get_adjusted_counts_for_unwanted_variation_bulk: no visible global
function definition for ‘all_of’
get_assay_scaled_if_exists_SE: no visible binding for global variable
‘tt_columns’
get_assay_scaled_if_exists_SE: no visible binding for global variable
‘.abundance_scaled’
get_cell_type_proportions: no visible binding for global variable ‘.’
get_clusters_SNN_bulk: no visible binding for global variable
‘seurat_clusters’
get_clusters_SNN_bulk_SE: no visible binding for global variable ‘.’
get_clusters_SNN_bulk_SE: no visible binding for global variable
‘seurat_clusters’
get_clusters_kmeans_bulk: no visible binding for global variable ‘.’
get_clusters_kmeans_bulk: no visible binding for global variable
‘cluster’
get_clusters_kmeans_bulk: no visible binding for global variable
‘cluster kmeans’
get_clusters_kmeans_bulk_SE: no visible binding for global variable ‘.’
get_clusters_kmeans_bulk_SE: no visible binding for global variable
‘cluster’
get_differential_transcript_abundance_bulk: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_bulk_SE: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_bulk_voom: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_bulk_voom_SE: no visible binding
for global variable ‘.’
get_differential_transcript_abundance_deseq2: no visible binding for
global variable ‘counts’
get_differential_transcript_abundance_deseq2: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_deseq2_SE: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_glmmSeq: no visible binding for
global variable ‘tagwise.dispersion’
get_differential_transcript_abundance_glmmSeq: no visible binding for
global variable ‘.’
get_differential_transcript_abundance_glmmSeq_SE: no visible binding
for global variable ‘tagwise.dispersion’
get_differential_transcript_abundance_glmmSeq_SE: no visible binding
for global variable ‘.’
get_reduced_dimensions_MDS_bulk: no visible binding for global variable
‘Component’
get_reduced_dimensions_MDS_bulk: no visible binding for global variable
‘Component value’
get_reduced_dimensions_MDS_bulk_SE: no visible binding for global
variable ‘Component’
get_reduced_dimensions_MDS_bulk_SE: no visible binding for global
variable ‘Component value’
get_reduced_dimensions_PCA_bulk: no visible binding for global variable
‘sdev’
get_reduced_dimensions_PCA_bulk: no visible binding for global variable
‘name’
get_reduced_dimensions_PCA_bulk: no visible binding for global variable
‘value’
get_reduced_dimensions_PCA_bulk: no visible binding for global variable
‘x’
get_reduced_dimensions_PCA_bulk_SE: no visible binding for global
variable ‘sdev’
get_reduced_dimensions_PCA_bulk_SE: no visible binding for global
variable ‘name’
get_reduced_dimensions_PCA_bulk_SE: no visible binding for global
variable ‘value’
get_reduced_dimensions_PCA_bulk_SE: no visible binding for global
variable ‘x’
get_reduced_dimensions_TSNE_bulk: no visible binding for global
variable ‘Y’
get_reduced_dimensions_TSNE_bulk_SE: no visible binding for global
variable ‘Y’
get_reduced_dimensions_UMAP_bulk_SE: no visible binding for global
variable ‘x’
get_rotated_dimensions: no visible binding for global variable ‘value’
get_rotated_dimensions: no visible binding for global variable ‘rotated
dimensions’
get_scaled_counts_bulk: no visible binding for global variable ‘med’
get_scaled_counts_bulk: no visible binding for global variable
‘tot_filt’
get_scaled_counts_bulk: no visible binding for global variable ‘nf’
get_scaled_counts_bulk: no visible binding for global variable ‘.’
get_scaled_counts_bulk: no visible binding for global variable ‘tot’
get_symbol_from_ensembl: no visible binding for global variable
‘ensembl_id’
get_symbol_from_ensembl: no visible binding for global variable
‘transcript’
get_symbol_from_ensembl: no visible binding for global variable
‘ref_genome’
get_tt_columns: no visible binding for global variable ‘tt_columns’
glmerCore: no visible global function definition for ‘coef’
glmerCore: no visible global function definition for ‘vcov’
glmerCore: no visible global function definition for ‘AIC’
glmerCore: no visible global function definition for ‘logLik’
glmerCore: no visible global function definition for ‘anova’
glmerCore: no visible global function definition for ‘predict’
glmmSeq: no visible global function definition for ‘update.formula’
glmmTMB_to_confidence_intervals_random_effects: no visible binding for
global variable ‘group_id’
glmmTMB_to_confidence_intervals_random_effects: no visible binding for
global variable ‘parameter’
glmmTMB_to_confidence_intervals_random_effects: no visible binding for
global variable ‘CI’
glmmTMB_to_confidence_intervals_random_effects: no visible binding for
global variable ‘lower’
glmmTMB_to_confidence_intervals_random_effects: no visible binding for
global variable ‘upper’
glmmTMBcore: no visible global function definition for ‘coef’
glmmTMBcore: no visible global function definition for ‘vcov’
glmmTMBcore: no visible global function definition for ‘AIC’
glmmTMBcore: no visible global function definition for ‘logLik’
glmmTMBcore: no visible global function definition for ‘anova’
glmmTMBcore: no visible global function definition for ‘predict’
initialise_tt_internals: no visible binding for global variable ‘.’
lmer_to_confidence_intervals_random_effects: no visible binding for
global variable ‘group_id’
lmer_to_confidence_intervals_random_effects: no visible binding for
global variable ‘parameter’
lmer_to_confidence_intervals_random_effects: no visible binding for
global variable ‘CI’
lmer_to_confidence_intervals_random_effects: no visible binding for
global variable ‘lower’
lmer_to_confidence_intervals_random_effects: no visible binding for
global variable ‘upper’
memorise_methods_used: no visible binding for global variable ‘.’
multivariable_differential_tissue_composition: no visible binding for
global variable ‘.’
multivariable_differential_tissue_composition: no visible binding for
global variable ‘.cell_type’
multivariable_differential_tissue_composition: no visible binding for
global variable ‘term’
multivariable_differential_tissue_composition_SE: no visible binding
for global variable ‘.’
multivariable_differential_tissue_composition_SE: no visible binding
for global variable ‘.cell_type’
multivariable_differential_tissue_composition_SE: no visible binding
for global variable ‘term’
remove_redundancy_elements_though_reduced_dimensions: no visible
binding for global variable ‘sample b’
remove_redundancy_elements_though_reduced_dimensions: no visible
binding for global variable ‘sample a’
remove_redundancy_elements_though_reduced_dimensions: no visible
binding for global variable ‘sample 1’
remove_redundancy_elements_though_reduced_dimensions: no visible
binding for global variable ‘sample 2’
remove_redundancy_elements_though_reduced_dimensions_SE: no visible
binding for global variable ‘sample b’
remove_redundancy_elements_though_reduced_dimensions_SE: no visible
binding for global variable ‘sample a’
remove_redundancy_elements_though_reduced_dimensions_SE: no visible
binding for global variable ‘sample 1’
remove_redundancy_elements_though_reduced_dimensions_SE: no visible
binding for global variable ‘sample 2’
remove_redundancy_elements_through_correlation: no visible binding for
global variable ‘rc’
remove_redundancy_elements_through_correlation: no visible binding for
global variable ‘transcript’
remove_redundancy_elements_through_correlation: no visible binding for
global variable ‘correlation’
remove_redundancy_elements_through_correlation: no visible binding for
global variable ‘item1’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘abundance’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘transcript’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘element’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘feature’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘rc’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘correlation’
remove_redundancy_elements_through_correlation_SE: no visible binding
for global variable ‘item1’
rowwise.tidybulk: no visible binding for global variable ‘.data’
run_epic: no visible global function definition for ‘EPIC’
run_llsr: no visible binding for global variable ‘X_cibersort’
scale_design: no visible binding for global variable ‘value’
scale_design: no visible binding for global variable ‘sample_idx’
scale_design: no visible binding for global variable ‘(Intercept)’
select_closest_pairs: no visible binding for global variable ‘sample 1’
select_closest_pairs: no visible binding for global variable ‘sample 2’
subset_tibble_output: no visible binding for global variable ‘.’
symbol_to_entrez: no visible binding for global variable
‘transcript_upper’
symbol_to_entrez: no visible binding for global variable ‘entrez’
test_differential_cellularity: no visible binding for global variable
‘X_cibersort’
test_differential_cellularity_: no visible binding for global variable
‘cell_type’
test_differential_cellularity_: no visible binding for global variable
‘prop’
test_differential_cellularity_: no visible binding for global variable
‘.’
test_differential_cellularity_: no visible binding for global variable
‘.cell_type’
test_gene_enrichment_bulk_EGSEA: no visible global function definition
for ‘buildCustomIdx’
test_gene_enrichment_bulk_EGSEA: no visible global function definition
for ‘buildIdx’
test_gene_enrichment_bulk_EGSEA: no visible binding for global variable
‘pathway’
test_gene_enrichment_bulk_EGSEA: no visible binding for global variable
‘data_base’
test_gene_enrichment_bulk_EGSEA: no visible binding for global variable
‘web_page’
test_gene_enrichment_bulk_EGSEA: no visible global function definition
for ‘egsea’
test_stratification_cellularity: no visible binding for global variable
‘X_cibersort’
test_stratification_cellularity_: no visible binding for global
variable ‘.cell_type’
tidybulk_to_SummarizedExperiment: no visible binding for global
variable ‘.’
univariable_differential_tissue_composition: no visible binding for
global variable ‘.proportion’
univariable_differential_tissue_composition: no visible binding for
global variable ‘.cell_type’
univariable_differential_tissue_composition: no visible binding for
global variable ‘cell_type_proportions’
univariable_differential_tissue_composition: no visible binding for
global variable ‘surv_test’
univariable_differential_tissue_composition_SE: no visible binding for
global variable ‘.proportion’
univariable_differential_tissue_composition_SE: no visible binding for
global variable ‘.cell_type’
univariable_differential_tissue_composition_SE: no visible binding for
global variable ‘cell_type_proportions’
univariable_differential_tissue_composition_SE: no visible binding for
global variable ‘surv_test’
univariable_differential_tissue_stratification: no visible binding for
global variable ‘.cell_type’
univariable_differential_tissue_stratification: no visible binding for
global variable ‘cell_type_proportions’
univariable_differential_tissue_stratification: no visible binding for
global variable ‘surv_test’
univariable_differential_tissue_stratification_SE: no visible binding
for global variable ‘.cell_type’
univariable_differential_tissue_stratification_SE: no visible binding
for global variable ‘cell_type_proportions’
univariable_differential_tissue_stratification_SE: no visible binding
for global variable ‘surv_test’
adjust_abundance,RangedSummarizedExperiment: no visible binding for
global variable ‘x’
adjust_abundance,SummarizedExperiment: no visible binding for global
variable ‘x’
aggregate_duplicates,RangedSummarizedExperiment: no visible binding for
global variable ‘group_name’
aggregate_duplicates,RangedSummarizedExperiment: no visible binding for
global variable ‘group’
aggregate_duplicates,SummarizedExperiment: no visible binding for
global variable ‘group_name’
aggregate_duplicates,SummarizedExperiment: no visible binding for
global variable ‘group’
describe_transcript,RangedSummarizedExperiment: no visible binding for
global variable ‘transcript’
describe_transcript,RangedSummarizedExperiment: no visible binding for
global variable ‘description’
describe_transcript,SummarizedExperiment: no visible binding for global
variable ‘transcript’
describe_transcript,SummarizedExperiment: no visible binding for global
variable ‘description’
identify_abundant,spec_tbl_df: no visible binding for global variable
‘.abundant’
identify_abundant,tbl_df: no visible binding for global variable
‘.abundant’
identify_abundant,tidybulk: no visible binding for global variable
‘.abundant’
keep_abundant,spec_tbl_df: no visible binding for global variable
‘.abundant’
keep_abundant,tbl_df: no visible binding for global variable
‘.abundant’
keep_abundant,tidybulk: no visible binding for global variable
‘.abundant’
pivot_sample,RangedSummarizedExperiment: no visible binding for global
variable ‘.’
pivot_sample,SummarizedExperiment: no visible binding for global
variable ‘.’
quantile_normalise_abundance,RangedSummarizedExperiment: no visible
binding for global variable ‘x’
quantile_normalise_abundance,SummarizedExperiment: no visible binding
for global variable ‘x’
quantile_normalise_abundance,spec_tbl_df: no visible binding for global
variable ‘x’
quantile_normalise_abundance,tbl_df: no visible binding for global
variable ‘x’
quantile_normalise_abundance,tidybulk: no visible binding for global
variable ‘x’
scale_abundance,RangedSummarizedExperiment: no visible binding for
global variable ‘x’
scale_abundance,SummarizedExperiment: no visible binding for global
variable ‘x’
scale_abundance,spec_tbl_df: no visible binding for global variable ‘x’
scale_abundance,spec_tbl_df: no visible binding for global variable
‘multiplier’
scale_abundance,tbl_df: no visible binding for global variable ‘x’
scale_abundance,tbl_df: no visible binding for global variable
‘multiplier’
scale_abundance,tidybulk: no visible binding for global variable ‘x’
scale_abundance,tidybulk: no visible binding for global variable
‘multiplier’
test_differential_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘X_cibersort’
test_differential_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘cell_type’
test_differential_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘prop’
test_differential_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘.cell_type’
test_differential_cellularity,SummarizedExperiment: no visible binding
for global variable ‘X_cibersort’
test_differential_cellularity,SummarizedExperiment: no visible binding
for global variable ‘cell_type’
test_differential_cellularity,SummarizedExperiment: no visible binding
for global variable ‘prop’
test_differential_cellularity,SummarizedExperiment: no visible binding
for global variable ‘.cell_type’
test_differential_cellularity,spec_tbl_df: no visible binding for
global variable ‘X_cibersort’
test_differential_cellularity,tbl_df: no visible binding for global
variable ‘X_cibersort’
test_differential_cellularity,tidybulk: no visible binding for global
variable ‘X_cibersort’
test_gene_enrichment,RangedSummarizedExperiment: no visible global
function definition for ‘buildCustomIdx’
test_gene_enrichment,RangedSummarizedExperiment: no visible global
function definition for ‘buildIdx’
test_gene_enrichment,RangedSummarizedExperiment: no visible global
function definition for ‘egsea’
test_gene_enrichment,RangedSummarizedExperiment: no visible binding for
global variable ‘pathway’
test_gene_enrichment,RangedSummarizedExperiment: no visible binding for
global variable ‘data_base’
test_gene_enrichment,RangedSummarizedExperiment: no visible binding for
global variable ‘web_page’
test_gene_enrichment,SummarizedExperiment: no visible global function
definition for ‘buildCustomIdx’
test_gene_enrichment,SummarizedExperiment: no visible global function
definition for ‘buildIdx’
test_gene_enrichment,SummarizedExperiment: no visible global function
definition for ‘egsea’
test_gene_enrichment,SummarizedExperiment: no visible binding for
global variable ‘pathway’
test_gene_enrichment,SummarizedExperiment: no visible binding for
global variable ‘data_base’
test_gene_enrichment,SummarizedExperiment: no visible binding for
global variable ‘web_page’
test_gene_overrepresentation,RangedSummarizedExperiment: no visible
binding for global variable ‘my_do_test’
test_gene_overrepresentation,SummarizedExperiment: no visible binding
for global variable ‘my_do_test’
test_gene_overrepresentation,spec_tbl_df: no visible binding for global
variable ‘my_do_test’
test_gene_overrepresentation,tbl_df: no visible binding for global
variable ‘my_do_test’
test_gene_overrepresentation,tidybulk: no visible binding for global
variable ‘my_do_test’
test_gene_rank,RangedSummarizedExperiment: no visible global function
definition for ‘desc’
test_gene_rank,SummarizedExperiment: no visible global function
definition for ‘desc’
test_gene_rank,spec_tbl_df: no visible global function definition for
‘with_groups’
test_gene_rank,spec_tbl_df: no visible global function definition for
‘desc’
test_gene_rank,tbl_df: no visible global function definition for
‘with_groups’
test_gene_rank,tbl_df: no visible global function definition for ‘desc’
test_gene_rank,tidybulk: no visible global function definition for
‘with_groups’
test_gene_rank,tidybulk: no visible global function definition for
‘desc’
test_stratification_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘X_cibersort’
test_stratification_cellularity,RangedSummarizedExperiment: no visible
binding for global variable ‘.cell_type’
test_stratification_cellularity,SummarizedExperiment: no visible
binding for global variable ‘X_cibersort’
test_stratification_cellularity,SummarizedExperiment: no visible
binding for global variable ‘.cell_type’
test_stratification_cellularity,spec_tbl_df: no visible binding for
global variable ‘X_cibersort’
test_stratification_cellularity,tbl_df: no visible binding for global
variable ‘X_cibersort’
test_stratification_cellularity,tidybulk: no visible binding for global
variable ‘X_cibersort’
Undefined global functions or variables:
(Intercept) . .abundance_scaled .abundant .cell_type .contrasts .data
.feature .proportion AIC CI Component Component value EPIC GeneID NUL
Status X_cibersort Y abundance action add_count all_of anova
buildCustomIdx buildIdx cell_type cell_type_proportions cluster
cluster kmeans coef correlation counts cov_data ct_data data_base
desc description egsea element ensembl_id entrez entrez_gene feature
fit geneID genes group group_id group_name gs_cat item1
library_size__ logLik lower m med multiplier my_do_test my_n n_aggr
name nf nulldist parameter pathway predict prop rc read count
ref_genome rotated dimensions sample 1 sample 2 sample a sample b
sample_idx samples sdev seurat_clusters surv_test tagwise.dispersion
temp term test tot tot_filt transcript transcript_upper tt_columns
update.formula upper value variable vcov web_page where with_groups x
Consider adding
importFrom("base", "sample")
importFrom("stats", "AIC", "anova", "coef", "kmeans", "logLik",
"predict", "update.formula", "vcov")
to your NAMESPACE file.
* checking Rd files ... NOTE
checkRd: (-1) remove_redundancy-methods.Rd:158-175: Lost braces
158 | select_closest_pairs = function(df) {
| ^
checkRd: (-1) remove_redundancy-methods.Rd:161-171: Lost braces
161 | while (df |> nrow() > 0) {
| ^
checkRd: (-1) rotate_dimensions-methods.Rd:126-134: Lost braces
126 | rotation = function(m, d) {
| ^
* 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 ... NOTE
Documented arguments not in \usage in Rd file 'get_reduced_dimensions_UMAP_bulk.Rd':
‘log_transform’
Documented arguments not in \usage in Rd file 'get_reduced_dimensions_UMAP_bulk_SE.Rd':
‘.abundance’ ‘.feature’ ‘.element’
Functions with \usage entries need to have the appropriate \alias
entries, and all their arguments documented.
The \usage entries must correspond to syntactically valid R code.
See chapter ‘Writing R documentation files’ in the ‘Writing R
Extensions’ manual.
* 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 LazyData ... OK
* checking data for ASCII and uncompressed saves ... OK
* checking files in ‘vignettes’ ... OK
* checking examples ... OK
Examples with CPU (user + system) or elapsed time > 5s
user system elapsed
test_differential_abundance-methods 72.603 0.644 82.980
test_differential_cellularity-methods 23.561 0.248 28.326
test_stratification_cellularity-methods 13.565 0.127 16.153
deconvolve_cellularity-methods 10.109 0.121 11.432
adjust_abundance-methods 8.288 0.307 9.578
* checking for unstated dependencies in ‘tests’ ... OK
* checking tests ...
Running ‘testthat.R’
OK
* checking for unstated dependencies in vignettes ... OK
* checking package vignettes ... 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
‘/Users/biocbuild/bbs-3.20-bioc/meat/tidybulk.Rcheck/00check.log’
for details.
tidybulk.Rcheck/00install.out
############################################################################## ############################################################################## ### ### Running command: ### ### /Library/Frameworks/R.framework/Resources/bin/R CMD INSTALL tidybulk ### ############################################################################## ############################################################################## * installing to library ‘/Library/Frameworks/R.framework/Versions/4.4-x86_64/Resources/library’ * installing *source* package ‘tidybulk’ ... ** using staged installation ** R ** data *** moving datasets to lazyload DB ** inst ** byte-compile and prepare package for lazy loading Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'expm1' Note: wrong number of arguments to 'floor' Note: wrong number of arguments to 'floor' ** help *** installing help indices *** copying figures ** 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 (tidybulk)
tidybulk.Rcheck/tests/testthat.Rout
R version 4.4.0 Patched (2024-04-24 r86482) -- "Puppy Cup"
Copyright (C) 2024 The R Foundation for Statistical Computing
Platform: x86_64-apple-darwin20
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(tidybulk)
Loading required package: ttservice
========================================
tidybulk version 1.17.0
If you use TIDYBULK in published research, please cite:
Mangiola et al. tidybulk: an R tidy framework for modular
transcriptomic data analysis. Genome Biology 2021.
This message can be suppressed by:
suppressPackageStartupMessages(library(tidybulk))
========================================
Attaching package: 'tidybulk'
The following object is masked from 'package:stats':
filter
>
> test_check("tidybulk")
Coefficients not estimable: conditionTRUE
Coefficients not estimable: conditionTRUE
Time difference of 4.801653 secs
Time difference of 4.732066 secs
Found 2 batches
Using null model in ComBat-seq.
Adjusting for 1 covariate(s) or covariate level(s)
Estimating dispersions
Fitting the GLM model
Apply shrinkage - computing posterior estimates for parameters
Using 100 random genes for Monte Carlo integration
Adjusting the data
Found 2 batches
Using null model in ComBat-seq.
Adjusting for 1 covariate(s) or covariate level(s)
Estimating dispersions
Fitting the GLM model
Apply shrinkage - computing posterior estimates for parameters
Using 100 random genes for Monte Carlo integration
Adjusting the data
Found 2 batches
Using null model in ComBat-seq.
Adjusting for 1 covariate(s) or covariate level(s)
Estimating dispersions
Fitting the GLM model
Apply shrinkage - computing posterior estimates for parameters
Using 100 random genes for Monte Carlo integration
Adjusting the data
Time difference of 12.7872 secs
Time difference of 12.06414 secs
Performing PCA
Read the 251 x 50 data matrix successfully!
Using no_dims = 2, perplexity = 30.000000, and theta = 0.500000
Computing input similarities...
Building tree...
Done in 0.05 seconds (sparsity = 0.490437)!
Learning embedding...
Iteration 50: error is 57.296347 (50 iterations in 0.06 seconds)
Iteration 100: error is 55.890843 (50 iterations in 0.07 seconds)
Iteration 150: error is 55.581122 (50 iterations in 0.08 seconds)
Iteration 200: error is 55.773826 (50 iterations in 0.07 seconds)
Iteration 250: error is 57.361411 (50 iterations in 0.07 seconds)
Iteration 300: error is 1.109711 (50 iterations in 0.07 seconds)
Iteration 350: error is 0.854477 (50 iterations in 0.06 seconds)
Iteration 400: error is 0.828505 (50 iterations in 0.05 seconds)
Iteration 450: error is 0.812710 (50 iterations in 0.05 seconds)
Iteration 500: error is 0.811128 (50 iterations in 0.05 seconds)
Iteration 550: error is 0.806837 (50 iterations in 0.05 seconds)
Iteration 600: error is 0.807974 (50 iterations in 0.05 seconds)
Iteration 650: error is 0.802660 (50 iterations in 0.05 seconds)
Iteration 700: error is 0.800443 (50 iterations in 0.05 seconds)
Iteration 750: error is 0.800163 (50 iterations in 0.05 seconds)
Iteration 800: error is 0.794675 (50 iterations in 0.05 seconds)
Iteration 850: error is 0.785426 (50 iterations in 0.05 seconds)
Iteration 900: error is 0.776196 (50 iterations in 0.05 seconds)
Iteration 950: error is 0.772181 (50 iterations in 0.05 seconds)
Iteration 1000: error is 0.772618 (50 iterations in 0.05 seconds)
Fitting performed in 1.12 seconds.
[ FAIL 0 | WARN 47 | SKIP 3 | PASS 225 ]
══ Skipped tests (3) ═══════════════════════════════════════════════════════════
• empty test (3): 'test-bulk_methods.R:1067:1',
'test-tximeta_GRnges_IRanges.R:3:1', 'test-tximeta_GRnges_IRanges.R:19:1'
[ FAIL 0 | WARN 47 | SKIP 3 | PASS 225 ]
>
> proc.time()
user system elapsed
421.668 12.075 515.659
tidybulk.Rcheck/tidybulk-Ex.timings
| name | user | system | elapsed | |
| adjust_abundance-methods | 8.288 | 0.307 | 9.578 | |
| aggregate_duplicates-methods | 0.188 | 0.003 | 0.211 | |
| arrange-methods | 0.019 | 0.006 | 0.025 | |
| as_matrix | 0.020 | 0.001 | 0.023 | |
| bind_rows | 0.615 | 0.032 | 0.721 | |
| cluster_elements-methods | 0.127 | 0.017 | 0.161 | |
| deconvolve_cellularity-methods | 10.109 | 0.121 | 11.432 | |
| describe_transcript-methods | 2.709 | 0.191 | 3.315 | |
| distinct-methods | 0.200 | 0.004 | 0.229 | |
| dplyr-methods | 0.445 | 0.012 | 0.512 | |
| ensembl_to_symbol-methods | 1.218 | 0.052 | 1.428 | |
| fill_missing_abundance-methods | 0.000 | 0.001 | 0.001 | |
| filter-methods | 0.605 | 0.008 | 0.694 | |
| get_bibliography-methods | 0.003 | 0.001 | 0.005 | |
| group_by-methods | 0.006 | 0.000 | 0.007 | |
| identify_abundant-methods | 0.033 | 0.003 | 0.049 | |
| impute_missing_abundance-methods | 0.195 | 0.002 | 0.224 | |
| join-methods | 1.954 | 0.028 | 2.151 | |
| keep_abundant-methods | 0.064 | 0.001 | 0.068 | |
| keep_variable-methods | 0.060 | 0.002 | 0.065 | |
| log10_reverse_trans | 0.372 | 0.012 | 0.437 | |
| logit_trans | 0.303 | 0.025 | 0.365 | |
| mutate-methods | 0.147 | 0.018 | 0.185 | |
| nest-methods | 1.073 | 0.087 | 1.307 | |
| pivot_sample-methods | 0.067 | 0.001 | 0.081 | |
| pivot_transcript-methods | 0.037 | 0.001 | 0.046 | |
| quantile_normalise_abundance-methods | 0.063 | 0.002 | 0.073 | |
| reduce_dimensions-methods | 0.402 | 0.005 | 0.457 | |
| remove_redundancy-methods | 0.586 | 0.034 | 0.849 | |
| rename-methods | 0.059 | 0.001 | 0.068 | |
| rotate_dimensions-methods | 0.213 | 0.004 | 0.244 | |
| rowwise-methods | 0.004 | 0.001 | 0.007 | |
| scale_abundance-methods | 0.145 | 0.002 | 0.162 | |
| summarise-methods | 0.005 | 0.000 | 0.005 | |
| symbol_to_entrez | 1.482 | 0.049 | 1.670 | |
| test_differential_abundance-methods | 72.603 | 0.644 | 82.980 | |
| test_differential_cellularity-methods | 23.561 | 0.248 | 28.326 | |
| test_gene_enrichment-methods | 0.000 | 0.001 | 0.002 | |
| test_gene_overrepresentation-methods | 0.001 | 0.001 | 0.002 | |
| test_gene_rank-methods | 0.000 | 0.001 | 0.002 | |
| test_stratification_cellularity-methods | 13.565 | 0.127 | 16.153 | |
| tidybulk-methods | 0.201 | 0.004 | 0.253 | |