Sailfish: Alignment-free Isoform Quantification from RNA-seq Reads using Lightweight Algorithms

(2) Department of Cell Biology; Carl Kingsford (1) ((1) Lane Center for Computational Biology; Carnegie Mellon University; Center for Bioinformatics; Computational Biology; Molecular Genetics; Rob Patro (1); School of Computer Science; Stephen M. Mount (2); University of Maryland)

arxiv: 1308.3700 · v1 · pith:P3AS4I2Znew · submitted 2013-08-16 · 🧬 q-bio.GN · cs.CE

Sailfish: Alignment-free Isoform Quantification from RNA-seq Reads using Lightweight Algorithms

Rob Patro (1) , Stephen M. Mount (2) , Carl Kingsford (1) ((1) Lane Center for Computational Biology , School of Computer Science , Carnegie Mellon University , (2) Department of Cell Biology , Molecular Genetics , Center for Bioinformatics

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Computational Biology University of Maryland)

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classification 🧬 q-bio.GN cs.CE

keywords sailfishrna-seqdatafasterquantificationreadsabundanceaccuracy

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RNA-seq has rapidly become the de facto technique to measure gene expression. However, the time required for analysis has not kept up with the pace of data generation. Here we introduce Sailfish, a novel computational method for quantifying the abundance of previously annotated RNA isoforms from RNA-seq data. Sailfish entirely avoids mapping reads, which is a time-consuming step in all current methods. Sailfish provides quantification estimates much faster than existing approaches (typically 20-times faster) without loss of accuracy.

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Sailfish: Alignment-free Isoform Quantification from RNA-seq Reads using Lightweight Algorithms

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