Mercurial > repos > george-weingart > graphlan_import
changeset 41:34a1b347e2e7 draft
Uploaded
| author | george-weingart |
|---|---|
| date | Sat, 06 Sep 2014 13:41:13 -0400 |
| parents | 4dc6abc28ba7 |
| children | fa2bd894219f |
| files | import2graphlan.xml |
| diffstat | 1 files changed, 23 insertions(+), 25 deletions(-) [+] |
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--- a/import2graphlan.xml Sat Sep 06 13:34:38 2014 -0400 +++ b/import2graphlan.xml Sat Sep 06 13:41:13 2014 -0400 @@ -78,8 +78,8 @@ <param name="most_abundant" type="integer" size="4" value="0" label=" When only lefse_input is provided, you can specify how many clades to highlight "/> <param name="least_biomarkers" type="integer" size="4" value="0" label="Minimum number of biomarkers to extract "/> <param name="discard_otus" type="select" label="If specified the OTU ids will be discarded from the taxonomy" value="0" > - <option value="0">Yes</option> - <option value="1">No</option> + <option value="0">No</option> + <option value="1">Yes</option> </param> @@ -109,11 +109,10 @@ * **Output of LEfSe**: This file is the result of LEfSe execute on the *Result of MetaPhlAn or HUMAnN analysis* file. This file allow GraPhlAn to highlight for you the found biomarkers. Input parameters +================ - --annotations ANNOTATIONS - List which levels should be annotated in the tree. Use - a comma separate values form, e.g., - --annotation_levels 1,2,3. Default is None + --annotations ANNOTATIONS List which levels should be annotated in the tree. Use a comma separate values form, e.g., -annotation_levels 1,2,3. Default is None + --external_annotations EXTERNAL_ANNOTATIONS List which levels should use the external legend for the annotation. Use a comma separate values form, @@ -179,31 +178,30 @@ the internal nodes - Input data matrix parameters: +Input data matrix parameters +============================ --sep SEP + --out_table OUT_TABLE : This is where to write the processed data matrix to file --fname_row FNAME_ROW : Row number containing the names of the features (default 0, specify -1 if no names are present in the matrix) - --sname_row SNAME_ROW - column number containing the names of the samples (default 0, specify -1 if no names are present in the matrix) - --metadata_rows METADATA_ROWS - Row numbers to use as metadata[default None, meaning - no metadata - --skip_rows SKIP_ROWS - Row numbers to skip (0-indexed, comma separated) from - the input file[default None, meaning no rows skipped - --sperc SPERC Percentile of sample value distribution for sample - selection - --fperc FPERC Percentile of feature value distribution for sample - selection - --stop STOP Number of top samples to select (ordering based on - percentile specified by --sperc) - --ftop FTOP Number of top features to select (ordering based on - percentile specified by --fperc) - --def_na DEF_NA Set the default value for missing values [default None - which means no replacement] + --sname_row SNAME_ROW column number containing the names of the samples (default 0, specify -1 if no names are present in the matrix) + + --metadata_rows METADATA_ROWS Row numbers to use as metadata[default None, meaning no metadata + + --skip_rows SKIP_ROWS Row numbers to skip (0-indexed, comma separated) from the input file[default None, meaning no rows skipped + + --sperc SPERC Percentile of sample value distribution for sample selection + + --fperc FPERC Percentile of feature value distribution for sample selection + + --stop STOP Number of top samples to select (ordering based on percentile specified by --sperc) + + --ftop FTOP Number of top features to select (ordering based on percentile specified by --fperc) + + --def_na DEF_NA Set the default value for missing values [default None which means no replacement] Integration ===========