A comparison of RNA-seq and exon arrays for whole genome transcription profiling of the L5 spinal nerve transection model of neuropathic pain in the rat

Conclusion: We recommend the use of RNA-seq for future high-throughput transcriptomic experiments in pain studies. RNA-seq allowed the identification of a larger number of putative candidate pain genes than microarrays and can also detect a wider range of expression values in a neuropathic pain model. In addition, RNA-seq can interrogate the whole genome regardless of prior annotations, being able to detect transcription from areas of the genome not currently annotated as exons. Some of these areas are differentially expressed following nerve injury, and may represent novel genes or isoforms. We also recommend the use of a high sequencing depth in order to detect differential expression for genes with low levels of expression.

http://www.molecularpain.com/content/10/1/7

Source: Molecular Pain - January 28, 2014 Category: Molecular Biology Authors: James PerkinsAna Antunes-MartinsMargarita CalvoJohn GristWerner RustRamona SchmidTobias HildebrandtMatthias KohlChristine OrengoStephen McMahonDavid Bennett Source Type: research