Hi,

I am new to NGS analysis and have been following this pipeline recommended in many of the posts in the forum.

I have 3 samples(1 child, 2 parents) and completed analysis till generation of VCF files. I couldn't understand clearly the VariantFiltration step from GATK documentation. Could someone please give more information on the same?

I would like to find de novo mutations in the child, Is it a good idea to proceed for de novo mutations identification after annotation or before annotation? Please advise me on how to proceed with this?

Thanks

Well, the filtering of the variant call is crucial step if you want to get the most accurate call. We have to deal with the probability that a SNP is a true genetic variant versus a sequencing or data processing artifact. Summarizing, you perform the filtering in order to discard false positive (increase specificity) variants without loosing true positive variants (sensitivity). GATK offers two approaches to do the filtering:

• VariantFiltration tool ---> Hard-filtering: Filter variants according to user defined criteria such as: depth (DP), quality (QUAL)...
• VariantRecalibrator + ApplyRecalibration tools : The first program assigns a well-calibrated probability to each variant call in a call set. The second program applies model parameters calculated by VariantRecalibrator to each variant in input VCF files producing a recalibrated VCF file in which each variant is annotated with its VQSLOD value. You can read more here: http://gatkforums.broadinstitute.org/discussion/39/variant-quality-score-recalibration-vqsr.

The first approach is the one one recommended in the pipeline you're following. But in my opinion that pipeline is a bit out of date. But you can just try both, and see the results and choose. Furthermore, in that pipeline, the variant call is performed using UnifiedGenotyper tool, and now there is one more updated tool in GATK that is HaplotypeCaller: https://www.broadinstitute.org/gatk/gatkdocs/org_broadinstitute_gatk_tools_walkers_haplotypecaller_HaplotypeCaller.php

Hope it helps.

If you are new to NGS I would suggest RTG Core (free for non-commercial use) which incorporates pedigree (trios/quads/multi-generation) directly into the variant calling, with automatic flagging of de novo candidates in the output VCF. The pipeline is very streamlined and includes all the steps that are usually separate stages of other pipelines:

1. rtg map each sample (results are pre-sorted and have calibration information determined)
2. rtg family (applies mapping calibration, identifies duplicates, calls variants, including realignment for haplotype calling, phased according to inheritance, and applies variant recalibration)
3. rtg vcffilter (isolate calls from the trio flagged as de-novo, with any extra filtering you might want to apply)