ovcCrijns: Function to compute the subtype scores and risk...
In bhklab/genefu: Computation of Gene Expression-Based Signatures in Breast Cancer
ovcCrijns R Documentation
Function to compute the subtype scores and risk classifications
for the prognostic signature published by Crinjs et al.
Description
This function computes subtype scores and risk classifications from gene
expression values using the weights published by Crijns et al.
Usage
ovcCrijns(data, annot, hgs,
gmap = c("entrezgene", "ensembl_gene_id", "hgnc_symbol", "unigene"),
do.mapping = FALSE, verbose = FALSE)
Arguments
data
Matrix of gene expressions with samples in rows and probes in
columns, dimnames being properly defined.
annot
Matrix of annotations with one column named as gmap, dimnames
being properly defined.
hgs
vector of booleans with TRUE represents the ovarian cancer
patients who have a high grade, late stage, serous tumor, FALSE otherwise.
This is particularly important for properly rescaling the data. If hgs is
missing, all the patients will be used to rescale the subtype score.
gmap
character string containing the biomaRt attribute to use for
mapping if do.mapping=TRUE
do.mapping
TRUE if the mapping through Entrez Gene ids must be
performed (in case of ambiguities, the most variant probe is kept for each
gene), FALSE otherwise.
verbose
TRUE to print informative messages, FALSE otherwise.
Details
Note that the original algorithm has not been implemented as it necessitates
refitting of the model weights in each new dataset. However the current
implementation should give similar results.
Value
A list with items:
score: Continuous signature scores.
risk: Binary risk classification, 1 being high risk and 0 being low risk.
mapping: Mapping used if necessary.
probe: If mapping is performed, this matrix contains the correspondence.
between the gene list (aka signature) and gene expression data.
References
Crijns APG, Fehrmann RSN, de Jong S, Gerbens F, Meersma G J, Klip HG,
Hollema H, Hofstra RMW, te Meerman GJ, de Vries EGE, van der Zee AGJ (2009)
"Survival-Related Profile, Pathways, and Transcription Factors in Ovarian
Cancer" PLoS Medicine, 6(2):e1000024.
See Also
sigOvcCrijns
Examples
# load the ovsCrijns signature
data(sigOvcCrijns)
# load NKI dataset
data(nkis)
colnames(annot.nkis)[is.element(colnames(annot.nkis), "EntrezGene.ID")] <-
"entrezgene"
# compute relapse score
ovcCrijns.nkis <- ovcCrijns(data=data.nkis, annot=annot.nkis,
gmap="entrezgene", do.mapping=TRUE)
table(ovcCrijns.nkis$risk)
bhklab/genefu documentation built on June 2, 2022, 2:56 p.m.
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
| ovcCrijns | R Documentation |
Function to compute the subtype scores and risk classifications for the prognostic signature published by Crinjs et al.
Description
This function computes subtype scores and risk classifications from gene expression values using the weights published by Crijns et al.
Usage
ovcCrijns(data, annot, hgs,
gmap = c("entrezgene", "ensembl_gene_id", "hgnc_symbol", "unigene"),
do.mapping = FALSE, verbose = FALSE)
Arguments
data |
Matrix of gene expressions with samples in rows and probes in columns, dimnames being properly defined. |
annot |
Matrix of annotations with one column named as gmap, dimnames being properly defined. |
hgs |
vector of booleans with TRUE represents the ovarian cancer patients who have a high grade, late stage, serous tumor, FALSE otherwise. This is particularly important for properly rescaling the data. If hgs is missing, all the patients will be used to rescale the subtype score. |
gmap |
character string containing the biomaRt attribute to use for mapping if do.mapping=TRUE |
do.mapping |
TRUE if the mapping through Entrez Gene ids must be performed (in case of ambiguities, the most variant probe is kept for each gene), FALSE otherwise. |
verbose |
TRUE to print informative messages, FALSE otherwise. |
Details
Note that the original algorithm has not been implemented as it necessitates refitting of the model weights in each new dataset. However the current implementation should give similar results.
Value
A list with items:
score: Continuous signature scores.
risk: Binary risk classification, 1 being high risk and 0 being low risk.
mapping: Mapping used if necessary.
probe: If mapping is performed, this matrix contains the correspondence. between the gene list (aka signature) and gene expression data.
References
Crijns APG, Fehrmann RSN, de Jong S, Gerbens F, Meersma G J, Klip HG, Hollema H, Hofstra RMW, te Meerman GJ, de Vries EGE, van der Zee AGJ (2009) "Survival-Related Profile, Pathways, and Transcription Factors in Ovarian Cancer" PLoS Medicine, 6(2):e1000024.
See Also
sigOvcCrijns
Examples
# load the ovsCrijns signature data(sigOvcCrijns) # load NKI dataset data(nkis) colnames(annot.nkis)[is.element(colnames(annot.nkis), "EntrezGene.ID")] <- "entrezgene" # compute relapse score ovcCrijns.nkis <- ovcCrijns(data=data.nkis, annot=annot.nkis, gmap="entrezgene", do.mapping=TRUE) table(ovcCrijns.nkis$risk)
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
Embedding an R snippet on your website
Add the following code to your website.
For more information on customizing the embed code, read Embedding Snippets.