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view gemini_interactions.xml @ 3:184aa4e686e2 draft
planemo upload for repository https://github.com/galaxyproject/tools-iuc/tree/master/tools/gemini commit 1f7418d74c6fcd61a050106ca5f9b66ab9a4c33d
| author | iuc |
|---|---|
| date | Wed, 17 Oct 2018 13:33:09 -0400 |
| parents | 527c8e4a356f |
| children | a6d326ffbb72 |
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<tool id="gemini_@BINARY@" name="GEMINI @BINARY@" version="@VERSION@.0"> <description>Find genes among variants that are interacting partners</description> <macros> <import>gemini_macros.xml</import> <token name="@BINARY@">interactions</token> </macros> <expand macro="requirements" /> <expand macro="stdio" /> <expand macro="version_command" /> <command> <![CDATA[ gemini #if $annotation_databases: --annotation-dir "${annotation_databases.fields.path}" #end if #if $gene.gene_selector == 'lof': ## lof interactions is a separate program lof_interactions #else: ## use normal gemini interactions program @BINARY@ -g "${gene.gene}" #end if -r "${radius}" $variant_mode "${ infile }" > "${ outfile }" ]]> </command> <inputs> <expand macro="infile" /> <conditional name="gene"> <param name="gene_selector" type="select" label="Studying" help=""> <option value="gene">Interesting gene</option> <option value="lof">All loss-of-function variants</option> </param> <when value="gene"> <param name="gene" type="text" label="Specify gene name" help="e.g. PTPN22 (-g)" /> </when> <when value="lof"/> </conditional> <expand macro="annotation_dir" /> <expand macro="radius" /> <expand macro="variant_mode" /> </inputs> <outputs> <data name="outfile" format="tabular" /> </outputs> <tests> <test> <param name="infile" value="gemini_burden_input.db" ftype="gemini.sqlite" /> <param name="gene" value="CTBP2" /> <param name="radius" value="5" /> <output name="outfile" file="gemini_interactions_result.tabular" /> </test> </tests> <help><![CDATA[ **What it does** Integrating the knowledge of the known protein-protein interactions would be useful in explaining variation data. Meaning to say that a damaging variant in an interacting partner of a potential protein may be equally interesting as the protein itself. We have used the HPRD_ binary interaction data to build a p-p network graph which can be explored by GEMINI. .. _HPRD: http://www.ncbi.nlm.nih.gov/pubmed/18988627 **Details** *interactions: Find genes among variants that are interacting partners.* Integrating the knowledge of the known protein-protein interactions would be useful in explaining variation data. Meaning to say that a damaging variant in an interacting partner of a potential protein may be equally interesting as the protein itself. We have used the HPRD binary interaction data to build a p-p network graph which can be explored by GEMINI. **Examples** EXAMPLE with setting -g CTBP2 and -r 3:: sample gene order_of_interaction interacting_gene M128215 CTBP2 0_order: CTBP2 M128215 CTBP2 1_order: RAI2 M128215 CTBP2 2_order: RB1 M128215 CTBP2 3_order: TGM2,NOTCH2NL Return CTBP2 (-g) interacting gene variants till the third order (-r) EXAMPLE lof_interactions (use this option to restrict your analysis to only LoF variants); lof_interactions and -r 3:: sample lof_gene order_of_interaction interacting_gene M128215 TGM2 1_order: RB1 M128215 TGM2 2_order: none M128215 TGM2 3_order: NOTCH2NL,CTBP2 Meaning to say return all LoF gene TGM2 (in sample M128215) interacting partners to a 3rd order of interaction. EXAMPLE --var. An extended variant information (chrom, start, end etc.) for the interacting gene may be achieved with the –var option for both the interactions and the lof_interactions. Settings '-g CTBP2', '-r 3' and '--var':: sample gene order_of_interaction interacting_gene var_id chrom start end impact biotype in_dbsnp clinvar_sig clinvar_disease_name aaf_1kg_all aaf_esp_all M128215 CTBP2 0 CTBP2 5 chr10 126678091 126678092 stop_gain protein_coding 1 None None None None M128215 CTBP2 1 RAI2 9 chrX 17819376 17819377 non_syn_coding protein_coding 1 None None 1 0.000473 M128215 CTBP2 2 RB1 7 chr13 48873834 48873835 upstream protein_coding 1 None None 0.94 None M128215 CTBP2 3 NOTCH2NL 1 chr1 145273344 145273345 non_syn_coding protein_coding 1 None None None None M128215 CTBP2 3 TGM2 8 chr20 36779423 36779424 stop_gain protein_coding 0 None None None None EXAMPLE with the following settings; '-r 3', '--var':: sample lof_gene order_of_interaction interacting_gene var_id chrom start end impact biotype in_dbsnp clinvar_sig clinvar_disease_name aaf_1kg_all aaf_esp_all M128215 TGM2 1 RB1 7 chr13 48873834 48873835 upstream protein_coding 1 None None 0.94 None M128215 TGM2 3 NOTCH2NL 1 chr1 145273344 145273345 non_syn_coding protein_coding 1 None None None None M128215 TGM2 3 CTBP2 5 chr10 126678091 126678092 stop_gain protein_coding 1 None None None None ]]></help> <expand macro="citations"> <citation type="doi">10.1093/nar/gkn892</citation><!-- HPRD citation --> </expand> </tool>