Dear GATK staff,
i have 28 vcf files from 31 humans exome data, the output after GenotypeGVCF according to the targeted gene intervals shows very little variant in each vcf files , less than 200 or 60 which seems might create a less reliable Gaussian model in VQSR. Should i use Mergevcfs to combine the 31 vcf files into a single file before piped them into VQSR?
i have 28 vcf files from 31 humans exome data, the output after GenotypeGVCF according to the targeted gene intervals shows very little variant in each vcf files , less than 200 or 60 which seems might create a less reliable Gaussian model in VQSR. Should i use Mergevcfs to combine the 31 vcf files into a single file before piped them into VQSR?