PEMer: a computational framework with simulation-based error models for inferring genomic structural variants from massive paired-end sequencing data

Open Access

23 February 2009

journal article
software
Published by Springer Nature in Genome Biology

Vol. 10 (2) , 1-14
https://doi.org/10.1186/gb-2009-10-2-r23

Abstract

Personal-genomics endeavors, such as the 1000 Genomes project, are generating maps of genomic structural variants by analyzing ends of massively sequenced genome fragments. To process these we developed Paired-End Mapper (PEMer; http://sv.gersteinlab.org/pemer). This comprises an analysis pipeline, compatible with several next-generation sequencing platforms; simulation-based error models, yielding confidence-values for each structural variant; and a back-end database. The simulations demonstrated high structural variant reconstruction efficiency for PEMer's coverage-adjusted multi-cutoff scoring-strategy and showed its relative insensitivity to base-calling errors.

Keywords

This publication has 46 references indexed in Scilit:

Bioinformatics challenges of new sequencing technology
Published by Elsevier ,2008
The Fine-Scale and Complex Architecture of Human Copy-Number Variation
American Journal of Human Genetics, 2008
Diet and the evolution of human amylase gene copy number variation
Nature Genetics, 2007
Identification and analysis of functional elements in 1% of the human genome by the ENCODE pilot project
Nature, 2007
Global variation in copy number in the human genome
Nature, 2006
Genome assembly comparison identifies structural variants in the human genome
Nature Genetics, 2006
Copy number polymorphism in Fcgr3 predisposes to glomerulonephritis in rats and humans
Nature, 2006
A high-resolution survey of deletion polymorphism in the human genome
Nature Genetics, 2005
Fine-scale structural variation of the human genome
Nature Genetics, 2005
BLAT—The BLAST-Like Alignment Tool
Genome Research, 2002