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  • mpileup to STRUCTURE

    Hi all,
    Thought I would see if anyone has a different (better!) pipeline for collecting a set of SNPs from many bam files for use with STRUCTURE or other population genetic software. The end goal is to have a matrix with SNPs as rows and samples in column.

    Ex.
    x y z
    Site 1 T T G
    Site 2 G A C
    Site 3 A G G


    1. Create mpileup file
    2. Call SNPs (with your favorite software) for each sample
    3. Create merged SNP list, with the end of goal of having each position where there is a SNP in at least one sample
    4. Create consensus fasta file from mpileup for each sample
    5. Extract consensus nucleotide from each position (#3) from consensus fasta (#4)
    6. Merge files

    One problem is that some SNP sites found in particular samples may not pass quality filters in other samples. I would love to hear of other pipelines.

    Thanks!

  • #2
    Have you tried just sending the mpileup to bamtools call?
    samtools mpileup -gu -t DP -f ref.fasta -b bam_file_list.txt| bcftools call -cv - > genotypes.vcf
    You'll need to sort the bam files, with samtools sort for instance

    or the equivalent from freebayes
    freebayes -f $ref_fasta_file bam_string > vcf_name
    You'll need to "read group" the bams with bamaddrg -b bamfile and then index with bamtools index.

    Either of these should be filtered with vcftools or vcflib to keep the SNPs with a certain presence in the population, using calls of a certain depth for each sample, etc.
    Last edited by SNPsaurus; 08-11-2015, 07:30 PM.
    Providing nextRAD genotyping and PacBio sequencing services. http://snpsaurus.com

    Comment


    • #3
      Thanks for these suggestions. I actually haven't explored bcftools or freebayes so should have a busy few days

      I will post an update once I come to a satisfactory solution.

      Comment

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