Literature DB >> 24844236

Integrative RNA-seq and microarray data analysis reveals GC content and gene length biases in the psoriasis transcriptome.

William R Swindell1, Xianying Xing2, John J Voorhees2, James T Elder2, Andrew Johnston2, Johann E Gudjonsson2.   

Abstract

Gene expression profiling of psoriasis has driven research advances and may soon provide the basis for clinical applications. For expression profiling studies, RNA-seq is now a competitive technology, but RNA-seq results may differ from those obtained by microarray. We therefore compared findings obtained by RNA-seq with those from eight microarray studies of psoriasis. RNA-seq and microarray datasets identified similar numbers of differentially expressed genes (DEGs), with certain genes uniquely identified by each technology. Correspondence between platforms and the balance of increased to decreased DEGs was influenced by mRNA abundance, GC content, and gene length. Weakly expressed genes, genes with low GC content, and long genes were all biased toward decreased expression in psoriasis lesions. The strength of these trends differed among array datasets, most likely due to variations in RNA quality. Gene length bias was by far the strongest trend and was evident in all datasets regardless of the expression profiling technology. The effect was due to differences between lesional and uninvolved skin with respect to the genome-wide correlation between gene length and gene expression, which was consistently more negative in psoriasis lesions. These findings demonstrate the complementary nature of RNA-seq and microarray technology and show that integrative analysis of both data types can provide a richer view of the transcriptome than strict reliance on a single method alone. Our results also highlight factors affecting correspondence between technologies, and we have established that gene length is a major determinant of differential expression in psoriasis lesions.

Entities:  

Keywords:  RNase 7; RNase L; degradation; gene expression; ribonuclease

Mesh:

Substances:

Year:  2014        PMID: 24844236      PMCID: PMC4121624          DOI: 10.1152/physiolgenomics.00022.2014

Source DB:  PubMed          Journal:  Physiol Genomics        ISSN: 1094-8341            Impact factor:   3.107


  73 in total

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7.  Psoriasis drug development and GWAS interpretation through in silico analysis of transcription factor binding sites.

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9.  Proteogenomic analysis of psoriasis reveals discordant and concordant changes in mRNA and protein abundance.

Authors:  William R Swindell; Henriette A Remmer; Mrinal K Sarkar; Xianying Xing; Drew H Barnes; Liza Wolterink; John J Voorhees; Rajan P Nair; Andrew Johnston; James T Elder; Johann E Gudjonsson
Journal:  Genome Med       Date:  2015-08-04       Impact factor: 11.117

10.  NOD-like receptor signaling and inflammasome-related pathways are highlighted in psoriatic epidermis.

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