RNA-Seq for the identification of novel Mediator transcripts in endothelial progenitor cells.

Gene

Department of Biochemistry, Biophysics and General Pathology, Second University of Naples, Via L. De Crecchio 7, 80138 Naples, Italy; Institute of Diagnostic and Nuclear Development (SDN), IRCCS, Via E. Gianturco 113, 80143 Naples, Italy; U.O.C. Immunohematology, Transfusion Medicine and Transplant Immunology [SIMT], Regional Reference Laboratory of Transplant Immunology [LIT], Azienda Universitaria Policlinico (AOU), 1st School of Medicine, Second University of Naples, Piazza Miraglia 2, 80138 Naples, Italy.

Published: August 2014

AI Article Synopsis

  • The Mediator (MED) complex is crucial for transcription in eukaryotic cells, and changes in its function can lead to various human diseases.
  • This study utilized both computational and experimental methods to discover new transcripts from MED genes, specifically focusing on alternative splicing in endothelial progenitor cells (EPCs).
  • New transcripts were identified for several MED genes that may produce different protein isoforms, which could help classify cell populations involved in neovascularization and potentially reveal new MED complexes with distinct functions.

Article Abstract

Mediator (MED) complex is a multiprotein playing a key role in the eukaryotic transcription. Alteration of MED function may have enormous pathophysiological consequences and several MED genes have been implicated in human diseases. Here, we have combined computational and experimental approaches to identify and characterize, new transcripts generated by alternative splicing (AS) for all MED genes, through the analysis of our recently published RNA-Sequencing datasets of endothelial progenitor cells (EPCs). This combined strategy allowed us to identify novel transcripts for MED4, MED9, MED11, MED14, MED27 and CDK8 most of them generated by AS. All the newly identified transcripts, except MED11, are predicted to encode novel protein isoforms. The identification of novel MED variants could lead to the finding of other MED complexes with different functions depending on their subunit composition. Finally, the expression profile of all MED genes, together with an extensive gene expression analysis, may be useful to better classify the diverse subsets of cell populations that contribute to neovascularization.

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http://dx.doi.org/10.1016/j.gene.2014.06.034DOI Listing

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