Time-course analysis with limma for >3 time points
1
0
Entering edit mode
relathman ▴ 20
@relathman-11472
Last seen 6.5 years ago
Germany

Dear all,
I want to use limma for the analysis of changing values over time. My data set consists of 2 conditions and 9 evenly spread time points (without replicates) for each condition.

I have two biological questions that I would like to address:
1)    I want to identify genes whose values change significantly over time in one condition.
2)    I want to identify genes who respond differently over time in condition 2 compared to condition 1.

I read in the user’s guide concerning time-course experiments in one condition that this problem “can be viewed as a factorial experiment but a simpler approach is to use the group-mean parametrization.”
However, I am still not quite sure how the contrast matrix should look like.
The user’s guide explains that “Any two contrasts between the three times would give the same result.  The same gene list would be obtained had "wt.24hr-wt.0hr" been used in place of "wt.24hr-wt.6hr" for example.”
I have already read the question "Limma and time-course data" covering a similar problem but I am not sure whether I understood it correctly.
Does it suffice to fit one contrast for the end point and the start point as long as they span the entire time course as described here? Or should I make a pairwise comparison of the 8 later time points with the first one?

This is what I have:

lev <- c("cond1_t1","cond1_t2","cond1_t3","cond1_t4","cond1_t5","cond1_t6","cond1_t7","cond1_t8","cond1_t9","cond2_t1","cond2_t2","cond2_t3","cond2_t4","cond2_t5","cond2_t6","cond2_t7","cond2_t8","cond2_t9")

f <- factor(targets$Target, levels=lev)
design <- model.matrix(~0+f)
colnames(design) <- lev
fit <- lmFit(eset, design)

# identify genes whose values change significantly over time in condition 1
contr_cond1 <- makeContrasts("cond1_t9-cond1_t1", "cond1_t8-cond1_t1", "cond1_t7-cond1_t1", "cond1_t6-cond1_t1", "cond1_t5-cond1_t1", "cond1_t4-cond1_t1", "cond1_t3-cond1_t1", "cond1_t2-cond1_t1",  levels=design)

# identify genes whose values change significantly over time in condition 2
contr_cond2 <- makeContrasts("cond2_t9-cond2_t1", "cond2_t8-cond2_t1", "cond2_t7-cond2_t1", "cond2_t6-cond2_t1", "cond2_t5-cond2_t1", "cond2_t4-cond2_t1", "cond2_t3-cond2_t1", "cond2_t2-cond2_t1",  levels=design)

# identify genes who respond differently over time in condition 2 compared to condition 1
contr.dif <- makeContrasts(dif9 =(cond2_t9-cond2_t1)-(cond1_t9-cond1_t1), dif8 =(cond2_t8-cond2_t1)-(cond1_t8-cond1_t1), dif7 =(cond2_t7-cond2_t1)-(cond1_t7-cond1_t1), dif6 =(cond2_t6-cond2_t1)-(cond1_t6-cond1_t1), dif5 =(cond2_t5-cond2_t1)-(cond1_t5-cond1_t1), dif4 =(cond2_t4-cond2_t1)-(cond1_t4-cond1_t1), dif3 =(cond2_t3-cond2_t1)-(cond1_t3-cond1_t1), dif2 =(cond2_t2-cond2_t1)-(cond1_t2-cond1_t1), levels=design)

 

fit2_cond1 <- contrasts.fit(fit, contr_cond1)
fit2_cond2 <- contrasts.fit(fit, contr_cond2)
fit2_dif <- contrasts.fit(fit, contr_dif)

fit2_cond1 <- eBayes(fit2_cond1)
fit2_cond2 <- eBayes(fit2_cond2)
fit2_dif <- eBayes(fit2_dif)

topTableF(fit2_cond1, adjust="BH")
topTableF(fit2_cond2, adjust="BH")
topTableF(fit2_dif, adjust="BH")

Is this approach appropriate for my biological questions or is there a better way to do it?
I would be very grateful for any help.

Best
Rukeia

limma contrast matrix design matrix multiple time points timecourse • 3.4k views
ADD COMMENT
0
Entering edit mode
@james-w-macdonald-5106
Last seen 1 day ago
United States

For that number of time points (and the questions at hand) you are likely better off using a spline fit. See section 9.6.2 in the limma User's Guide.

ADD COMMENT
0
Entering edit mode

hi James, I'm wondering how you would approach the OP's question (assuming sample size is not an issue) to compute coefficients for conditions (cond1, cond2) and time (t1, t2)? I have posted this question in here too.

ADD REPLY

Login before adding your answer.

Traffic: 493 users visited in the last hour
Help About
FAQ
Access RSS
API
Stats

Use of this site constitutes acceptance of our User Agreement and Privacy Policy.

Powered by the version 2.3.6