se.exprs
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Mary Putt ▴ 40
@mary-putt-356
Last seen 10.2 years ago
Hi, I have a question about the output of se.exprs. I normalized a data set using expresso and the model from Irizarry et al (2003) Biostatistics paper. rma.dta<-expresso(raw.data, normalize.method="quantiles.robust", bkground.correct="rma", summary.method="medianpolish", pmcorrect.method="pmonly") I can extract the expression values using exprs.rma<-exprs(rma.dta) and could compute a sample standard deviation from se.rma<-sqrt(apply(exprs.rma, 1, var)). The square of this estimates the variance of the individual expression values. I can also extract the model-based estimate of the standard deviation from se.model.rma<-se.exprs(rma.dta) I'm not sure whether se.model.rma (squared) estimates the variance of the individual espression values. I have a pdf file that explains some of the notation if this is helpful--but it is too long to be accepted by standard bioconductor means--I can send to individuals if this is helpful. This question was motivated by my observation that the sample standard deviation is substantially larger than the model-based standard deviation in a dataset that I am working with. Many thanks in advance, Mary Putt -------------- next part -------------- A non-text attachment was scrubbed... Name: mputt.vcf Type: text/x-vcard Size: 173 bytes Desc: Card for mary putt Url : https://www.stat.math.ethz.ch/pipermail/bioconductor/attachments /20030706/e2f9e6bc/mputt.bin
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@rafael-a-irizarry-205
Last seen 10.2 years ago
what you did to get se.rma is correct if you believe each gene in raw.data is equally expressed across arrays, i.e. if the arrays are technical replicates. if not there are variances included in se.rma not included in se.model.rma. if you have technical replicates then if 1) the model assumed by rma is exactly right and 2) the number of arrays is very large then se.model.rma should be approximately equal to se.rma. i dont think you have either: the model assumed by rma is useful but not perfect and i doubt you have 100s of arrays. if you don't have tech reps you will have to adjusts the summary step with an appropriate model to get a more useful se.model.rma. using rlm instead of median polish gives more satisfying results. also notice that it is very common, not just for microarray data, that the sample standard deviations are larger than nominal standard deviation. for example: x <- matrix(rnorm(100000),10000,10) means <- apply(x,1,mean) nominal.sd <- apply(x,1,sd)/sqrt(10) sample.sd <- sd(means) ##percent sample.sd bigger than nonminal.sd should be about 53%-58% meansample.sd > nominal.sd) hope this helps, rafael On Sun, 6 Jul 2003, Mary Putt wrote: > Hi, > I have a question about the output of se.exprs. I normalized a data set > using expresso and the model from Irizarry et al (2003) Biostatistics > paper. > > rma.dta<-expresso(raw.data, normalize.method="quantiles.robust", > bkground.correct="rma", summary.method="medianpolish", > pmcorrect.method="pmonly") > > I can extract the expression values using > > exprs.rma<-exprs(rma.dta) > and could compute a sample standard deviation from > > se.rma<-sqrt(apply(exprs.rma, 1, var)). The square of this estimates the > > variance of the individual expression values. > > I can also extract the model-based estimate of the standard deviation > from > > se.model.rma<-se.exprs(rma.dta) > > I'm not sure whether se.model.rma (squared) estimates the variance of > the individual espression values. I have a pdf file that explains some > of the notation if this is helpful--but it is too long to be accepted by > standard bioconductor means--I can send to individuals if this is > helpful. > > > This question was motivated by my observation that the sample standard > deviation is substantially larger than the model-based standard > deviation in a dataset that I am working with. > > Many thanks in advance, Mary Putt >
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Hi, I've been experimenting with the heatmap function of the mva library and am not happy with the ordering I get. Does anyone have a good suggestion? Or could you point me to a documentation of Jonathan Eisen's ordering algorithm? Many thanks in advance, Hinnerk
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Hinnerk , the arguments Colv and Rowv allow you to specify your own ordering on a different variable, I have done this on a phenotypic variable and seems to work very well, what exactly are you not happy about? Do you need a multivariate ranking procedure? Susan Holmes Statistics Stanford
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