how to find if an observed missense SNV is true observation and significant in targeted sequencing of few (5 or less) genes.

0

Entering edit mode

7.2 years ago

oriolebaltimore ▴ 190

Dear group, What are the methods/tests/algorithms that are available to find whether an observed missense/or any other SNV as significant variant among many cases (for a long genes, I am observing at least 10 missense and 10 synonymous variants).

If full genome or exome data is available, one would do mutsig2 etc. to test if observed SNV is by chance or ranks above background threshold. How do we deal with cases with VCF files and BAM files in hand. I am asking in the context of 4 genes, sequenced through amplicons from fluidigm/miseq setting.

Appreciate any input. thanks Adrian

next-gen sequencing targeted panels mutations • 1.4k views

ADD COMMENT • link updated 7.1 years ago by Biostar 20 • written 7.2 years ago by oriolebaltimore ▴ 190

0

Entering edit mode

this is not clear: " find whether an observed missense/or any other SNV as significant variant among many cases " what are you trying to do ??

ADD REPLY • link 7.2 years ago by karl.stamm 4.1k

0

Entering edit mode

Are you comparing patient samples with healthy control samples? Because that would make this an association analysis and you could either do a fisher exact test (e.g. in plink) or do a gene burden analysis/rare variant association analysis (e.g. in SKAT).

ADD REPLY • link 7.2 years ago by WouterDeCoster 47k

Login before adding your answer.