We are doing targeted exome sequencing with variant calling, and need to determine the minimum number of reads required to be 95% certain that a variant is not present in a given target region. How do you typically do that?
I was thinking some type of power analysis, but wasn't sure what values to use for which parameters.
Are there other ways to do this?
I assume you are talking about heterozygous sites. If we live in a perfect world where we sample each chromosome with p=1/2, at a coverage of 5X, you will only observe one particular allele with p=(1/2)^5 = 0.03125. So only observing one allele but not the other is twice that.
However, having observed a divergent base is not an immediate indicator of a variant. It could be due to mismapping, sequencing error, residual adapter, some contamination etc.
Genotypers are usually equipped to quantify your belief in a particular genotype versus another. I suggest that you look at genotyping output at various coverage and think about the confidence you want for a particular genotype.
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This has been done: https://www.ncbi.nlm.nih.gov/pubmed/23773188
Thanks for the link. Just curious, did you have this on hand, or did you find it on Google? I spent some time trying to Google this topic but did not find this paper, must have been using the wrong keywords :)
I knew it existed, from a couple of years ago. I faintly remembered the first author's name. No idea how I found it originally.