kda2cytoscape.drivers: Select top key drivers for each module
In zeynebkurtUCLA/Mergeomics: Integrative network analysis of omics data
Description
Usage
Arguments
Value
Author(s)
References
See Also
Examples
Description
kda2cytoscape.drivers finds maximally top ndriv key drivers
for each module with respect to the significance level of the drivers.
Usage
1
kda2cytoscape.drivers(data, modules, ndriv)
Arguments
data
data frame including information of the modules (key driver list,
p-values, node list, false discovery rates (fdr), and so on.)
modules
top scoring modules among KDA results
ndriv
maximum number of drivers that can be chosen for per module
Value
data
top key drivers (maximally ndriv drivers for each
module) for top modules
Author(s)
Zeyneb Kurt
References
Shu L, Zhao Y, Kurt Z, Byars SG, Tukiainen T, Kettunen J, Orozco LD,
Pellegrini M, Lusis AJ, Ripatti S, Zhang B, Inouye M, Makinen V-P, Yang X.
Mergeomics: multidimensional data integration to identify pathogenic
perturbations to biological systems. BMC genomics. 2016;17(1):874.
See Also
Examples
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## get the prepared and KDA applied dataset:(see kda.analyze for details)
data(job_kda_analyze)
## set the relevant parameters:
job.kda$label<-"HDLC"
## parent folder for results
job.kda$folder<-"Results"
## Input a network
## columns: TAIL HEAD WEIGHT
job.kda$netfile<-system.file("extdata","network.mouseliver.mouse.txt",
package="Mergeomics")
## Gene sets derived from ModuleMerge, containing two columns, MODULE,
## NODE, delimited by tab
job.kda$modfile<- system.file("extdata","mergedModules.txt",
package="Mergeomics")
## "0" means we do not consider edge weights while 1 is opposite.
job.kda$edgefactor<-0.0
## The searching depth for the KDA
job.kda$depth<-1
## 0 means we do not consider the directions of the regulatory interactions
## while 1 is opposite.
job.kda$direction <- 1
## Finish the KDA process
job.kda <- kda.finish(job.kda)
## Select top key drivers from each module.
## First, take module names from kda results
modules <- unique(job.kda$results$MODULE)
## Take top 2 KDs:
drivers <- kda2cytoscape.drivers(job.kda$results, modules, ndriv=2)
## remove the results folder
unlink("Results", recursive = TRUE)
zeynebkurtUCLA/Mergeomics documentation built on May 14, 2019, 1:59 a.m.
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Description Usage Arguments Value Author(s) References See Also Examples
Description
kda2cytoscape.drivers finds maximally top ndriv key drivers
for each module with respect to the significance level of the drivers.
Usage
1 | kda2cytoscape.drivers(data, modules, ndriv)
|
Arguments
data |
data frame including information of the modules (key driver list, p-values, node list, false discovery rates (fdr), and so on.) |
modules |
top scoring modules among KDA results |
ndriv |
maximum number of drivers that can be chosen for per module |
Value
data |
top key drivers (maximally |
Author(s)
Zeyneb Kurt
References
Shu L, Zhao Y, Kurt Z, Byars SG, Tukiainen T, Kettunen J, Orozco LD, Pellegrini M, Lusis AJ, Ripatti S, Zhang B, Inouye M, Makinen V-P, Yang X. Mergeomics: multidimensional data integration to identify pathogenic perturbations to biological systems. BMC genomics. 2016;17(1):874.
See Also
Examples
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 | ## get the prepared and KDA applied dataset:(see kda.analyze for details)
data(job_kda_analyze)
## set the relevant parameters:
job.kda$label<-"HDLC"
## parent folder for results
job.kda$folder<-"Results"
## Input a network
## columns: TAIL HEAD WEIGHT
job.kda$netfile<-system.file("extdata","network.mouseliver.mouse.txt",
package="Mergeomics")
## Gene sets derived from ModuleMerge, containing two columns, MODULE,
## NODE, delimited by tab
job.kda$modfile<- system.file("extdata","mergedModules.txt",
package="Mergeomics")
## "0" means we do not consider edge weights while 1 is opposite.
job.kda$edgefactor<-0.0
## The searching depth for the KDA
job.kda$depth<-1
## 0 means we do not consider the directions of the regulatory interactions
## while 1 is opposite.
job.kda$direction <- 1
## Finish the KDA process
job.kda <- kda.finish(job.kda)
## Select top key drivers from each module.
## First, take module names from kda results
modules <- unique(job.kda$results$MODULE)
## Take top 2 KDs:
drivers <- kda2cytoscape.drivers(job.kda$results, modules, ndriv=2)
## remove the results folder
unlink("Results", recursive = TRUE)
|
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