Entering edit mode
6 months ago
garcesj
▴
50
Hi,
I have performed whole-genome sequencing (WGS) in two different conditions: condA (n = 15) and condB (n = 23). I want to compare the number of mutations, but obviously, the different numbers of samples in each condition bias this number.
Is there a way of "correcting" by the number of samples? Note I don't want to take just the average (ie, total mutations/total samples condX) but "correct" the number of mutations in each different sample.
I tried just doing number of mutations in each sample/total samples condX, but something doesn't make sense to me.
Thanks a lot!
This comparison will give you literally no useful information.
How come? If I have a pro-tumorigenic product, for example, wouldn't this comparison be valid?
Something with 4 mutations need not be worse than something with 1. It depends on the effects of those mutations as well as other mitigating factors. Mut vs WT is a valid comparison, comparing number of mutations is not.
Or maybe you're on to something and I'm missing a critical component of your analysis.
I see your point, especially depending on affected genes, totally agree. However, differential values in the number of aberrations (in the broad sense, eg TMB, chromothripsis, etc.) seem to have a relevant value... or maybe I'm misunderstanding something?