Dear everyone,

I have been asked to comment on an experiment design that involves WES or WGS of cancer cell lines which lack matched normal.

I know that this design is far from ideal, but I was wondering if there are people who have already stream-lined it (to the extent possible of course). I can think of a couple of common variation filters to keep out the germline variants, but I am not sure how to go beyond.

I am sorry if this is a duplicate question; I couldn't find a related hit.

Thank you,

Noushin

The bottom line is that without a matched normal, you're just not going to be able to call the somatic status for the vast majority of sites. That said, you can winnow down a list to those you *suspect* are somatic. Some ideas:

• Weed out sites with high frequency in the population
• If your tumor is very impure, you can take advantage of the fact that the frequencies of somatic variants will be shifted away from 50%/100%

Since you are asking about cell lines, maybe these have already been sequenced. There are bigger studies I'm aware of:

1. Cancer Cell Line Encyclopedia (CCLE), see http://www.ncbi.nlm.nih.gov/pubmed/22460905
   Browse and download the data: http://www.broadinstitute.org/ccle/home
2. NCI-60 cell line, see e.g. here: http://www.cbioportal.org/public-portal/study.do?cancer_study_id=cellline_nci60

Then I would check against COSMIC for known somatic mutations. And maybe the cell line in question even has data in COSMIC, see By Sample at http://cancer.sanger.ac.uk/cancergenome/projects/cosmic/