English

SAMBLASTER: fast duplicate marking and structural variant read extraction

Genomics 2014-09-09 v1

Abstract

Motivation: Illumina DNA sequencing is now the predominant source of raw genomic data, and data volumes are growing rapidly. Bioinformatic analysis pipelines are having trouble keeping pace. A common bottleneck in such pipelines is the requirement to read, write, sort and compress large BAM files multiple times. Results: We present SAMBLASTER, a tool that reduces the number of times such costly operations are performed. SAMBLASTER is designed to mark duplicates in read-sorted SAM files as a piped post-pass on DNA aligner output before it is compressed to BAM. In addition, it can simultaneously output into separate files the discordant read-pairs and/or split-read mappings used for structural variant calling. As an alignment post-pass, its own runtime overhead is negligible, while dramatically reducing overall pipeline complexity and runtime. As a stand-alone duplicate marking tool, it performs significantly better than PICARD or SAMBAMBA in terms of both speed and memory usage, while achieving nearly identical results. Availability: SAMBLASTER is open source C++ code and freely available from https://github.com/GregoryFaust/samblaster

Keywords

Cite

@article{arxiv.1403.7486,
  title  = {SAMBLASTER: fast duplicate marking and structural variant read extraction},
  author = {Gregory G. Faust and Ira M. Hall},
  journal= {arXiv preprint arXiv:1403.7486},
  year   = {2014}
}
R2 v1 2026-06-22T03:37:33.957Z