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In silico transcriptional analysis of mRNA and miRNA reveals unique biosignatures that characterizes different types of diabetes

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Listed:
  • Juan M Cubillos-Angulo
  • Caian L Vinhaes
  • Eduardo R Fukutani
  • Victor V S Albuquerque
  • Artur T L Queiroz
  • Bruno B Andrade
  • Kiyoshi F Fukutani

Abstract

Diabetes (DM) has a significant impact on public health. We performed an in silico study of paired datasets of messenger RNA (mRNA) micro-RNA (miRNA) transcripts to delineate potential biosignatures that could distinguish prediabetes (pre-DM), type-1DM (T1DM) and type-2DM (T2DM). Two publicly available datasets containing expression values of mRNA and miRNA obtained from individuals diagnosed with pre-DM, T1DM or T2DM, and normoglycemic controls (NC), were analyzed using systems biology approaches to define combined signatures to distinguish different clinical groups. The mRNA profile of both pre-DM and T2DM was hallmarked by several differentially expressed genes (DEGs) compared to NC. Nevertheless, T1DM was characterized by an overall low number of DEGs. The miRNA signature profiles were composed of a substantially lower number of differentially expressed targets. Gene enrichment analysis revealed several inflammatory pathways in T2DM and fewer in pre-DM, but with shared findings such as Tuberculosis. The integration of mRNA and miRNA datasets improved the identification and discriminated the group composed by pre-DM and T2DM patients from that constituted by normoglycemic and T1DM individuals. The integrated transcriptomic analysis of mRNA and miRNA expression revealed a unique biosignature able to characterize different types of DM.

Suggested Citation

  • Juan M Cubillos-Angulo & Caian L Vinhaes & Eduardo R Fukutani & Victor V S Albuquerque & Artur T L Queiroz & Bruno B Andrade & Kiyoshi F Fukutani, 2020. "In silico transcriptional analysis of mRNA and miRNA reveals unique biosignatures that characterizes different types of diabetes," PLOS ONE, Public Library of Science, vol. 15(9), pages 1-17, September.
  • Handle: RePEc:plo:pone00:0239061
    DOI: 10.1371/journal.pone.0239061
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