International Journal of Molecular Sciences (Mar 2024)

Familial Dilated Cardiomyopathy: A Novel MED9 Short Isoform Identification

  • Monica Franzese,
  • Mario Zanfardino,
  • Andrea Soricelli,
  • Annapaola Coppola,
  • Ciro Maiello,
  • Marco Salvatore,
  • Concetta Schiano,
  • Claudio Napoli

DOI
https://doi.org/10.3390/ijms25053057
Journal volume & issue
Vol. 25, no. 5
p. 3057

Abstract

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Familial dilated cardiomyopathy (DCM) is among the leading indications for heart transplantation. DCM alters the transcriptomic profile. The alteration or activation/silencing of physiologically operating transcripts may explain the onset and progression of this pathological state. The mediator complex (MED) plays a fundamental role in the transcription process. The aim of this study is to investigate the MED subunits, which are altered in DCM, to identify target crossroads genes. RNA sequencing allowed us to identify specific MED subunits that are altered during familial DCM, transforming into human myocardial samples. N = 13 MED subunits were upregulated and n = 7 downregulated. MED9 alone was significantly reduced in patients compared to healthy subjects (HS) (FC = −1.257; p p p < 0.05), showing an increased MED9s isoform in DCM patients with respect to its full-length transcript. MED9 and GATA4 shared the same sequence motif and were involved in a network with FOG2/ZFPM2, FOS, and ID2, proteins already implicated in cardiac development.

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