VEP (Variant Effect Predictor) predicts the functional effects of genomic variants. The annotated VCF will be converted into MAF based on vcf2maf.
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  1. task VEP {
  2. File vcf
  3. String sample_id
  4. String basename = basename(vcf,".vcf")
  5. String tumor_id
  6. String normal_id
  7. File ref_dir
  8. String fasta
  9. String vep_path
  10. File cache
  11. String ncbi_build
  12. String species
  13. String vcf2maf_path
  14. String docker
  15. String cluster_config
  16. String disk_size
  17. command <<<
  18. set -o pipefail
  19. set -e
  20. nt=$(nproc)
  21. awk -F'\t' '{if(($1~"^#")||($1!~"^#" && $7=="PASS")){print $0}}' ${vcf} > ${sample_id}.vcf
  22. # Judge the SAMPLE info of vcf file
  23. ncol=`awk -F'\t' '{if($1!~"^#"){print NF}}' ${sample_id}.vcf | uniq`
  24. if [ $ncol -lt 11 ]; then
  25. SAMPLE="--tumor-id ${tumor_id} --normal-id ${normal_id}"
  26. else
  27. SAMPLE="--tumor-id ${sample_id}"
  28. fi
  29. # Set the buffer_size based on the data size
  30. nrow=`awk -F'\t' '{if($1~"^chr"){print $0}}' ${sample_id}.vcf | wc -l`
  31. if [ $nrow -lt 5000 ]; then
  32. buffer_size="--buffer_size 5000"
  33. else
  34. buffer_size="--buffer_size 1000"
  35. fi
  36. # Extract the BND variants from VCF
  37. # awk -F'\t' '{if(($1~"^#")||($8!~".*SVTYPE=BND.*")){print $0}}' ${sample_id}.PASS.vcf > ${sample_id}.PASS.vcf2maf.vcf
  38. # awk -F'\t' '{if(($1~"^#")||($8~".*SVTYPE=BND.*")){print $0}}' ${sample_id}.PASS.vcf > ${sample_id}.INPUT.VEP.vcf
  39. # vcf2maf
  40. # perl ${vcf2maf_path}/vcf2maf.pl \
  41. # --input-vcf ${sample_id}.PASS.vcf2maf.vcf --output-maf ${basename}.maf \
  42. # --tumor-id ${tumor_id} --normal-id ${normal_id} \
  43. # --ref-fasta ${ref_dir}/${fasta} \
  44. # --vep-path ${vep_path} \
  45. # --vep-data ${cache} \
  46. # --ncbi-build ${ncbi_build} \
  47. # --species ${species} \
  48. # --vep-fork $nt
  49. # vep
  50. # perl ${vep_path}/vep \
  51. # --input_file ${sample_id}.vcf --output_file ${basename}.PASS.vep.vcf \
  52. # --fasta ${ref_dir}/${fasta} \
  53. # --dir ${cache} \
  54. # --assembly ${ncbi_build} \
  55. # --species ${species} \
  56. # --fork $nt \
  57. # --format vcf --vcf \
  58. # --no_progress \
  59. # --no_stats \
  60. # $buffer_size \
  61. # --sift b \
  62. # --ccds --uniprot --hgvs --symbol --numbers --domains --gene_phenotype --canonical --protein --biotype --uniprot --tsl --variant_class --shift_hgvs 1 --check_existing --total_length --allele_number --no_escape --xref_refseq --failed 1 --flag_pick_allele --pick_order canonical,tsl,biotype,rank,ccds,length --force_overwrite --offline --pubmed --regulatory
  63. # vcf2vcf: transfer into a standardized format
  64. perl ${vcf2maf_path}/vcf2vcf.pl \
  65. --input-vcf ${sample_id}.vcf --output-vcf ${basename}.norm.vcf \
  66. $SAMPLE \
  67. --ref-fasta ${reference}
  68. # VEP annotation
  69. perl ${vep_path}/vep --format vcf --vcf \
  70. --assembly ${ncbi_build} \
  71. --species ${species} \
  72. --everything --af_exac \
  73. --offline \
  74. --cache --dir_cache ${cache} \
  75. --fasta ${ref_dir}/${fasta} \
  76. $buffer_size \
  77. --input_file ${basename}.norm.vcf --output_file ${basename}.vep.vcf
  78. # vcf2maf
  79. perl ${vcf2maf_path}/vcf2maf.pl \
  80. --inhibit-vep \
  81. --input-vcf ${basename}.vep.vcf --output-maf ${basename}.maf \
  82. $SAMPLE \
  83. --ref-fasta ${ref_dir}/${fasta} \
  84. --ncbi-build ${ncbi_build} \
  85. --species ${species} \
  86. --vep-fork $nt
  87. >>>
  88. runtime {
  89. docker: docker
  90. cluster: cluster_config
  91. systemDisk: "cloud_ssd 40"
  92. dataDisk: "cloud_ssd " + disk_size + " /cromwell_root/"
  93. }
  94. output {
  95. File vep_vcf = "${basename}.vep.vcf"
  96. File maf = "${basename}.maf"
  97. }
  98. }