BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs2476601, BRAF, Metabolism of xenobiotics, Inflammatory disorder, Heart, Vitamin E)
Bookmark Forward

T3 Critically Affects the Mhrt/Brg1 Axis to Regulate the Cardiac MHC Switch: Role of an Epigenetic Cross-Talk.

Francesca Forini, Giuseppina Nicolini, Claudia Kusmic, Romina D'Aurizio, Alberto Mercatanti, Giorgio Iervasi, Letizia Pitto

Cells 2020 Sep 24


filter terms:
  • Brg1 (9)
  • chromatin (3)
  • dna helicases (2)
  • factors (3)
  • heart (11)
  • ischemia (2)
  • isoform (1)
  • mirnas (1)
  • mutagenesis (1)
  • my (11)
  • Myh (3)
  • Myh6 (2)
  • Myh7 (2)
  • Myosin (2)
  • newborn (1)
  • protein rat (1)
  • rat (2)
  • rats wistar (1)
  • rna (3)
  • t3 has (1)
  • α myosin (1)
  • β myosin (1)
    • Sizes of these terms reflect their relevance to your search.

    The LncRNA my-heart (Mhrt) and the chromatin remodeler Brg1 inhibit each other to respectively prevent or favor the maladaptive α-myosin-heavy-chain (Myh6) to β-myosin-heavy-chain (Myh7) switch, so their balance crucially guides the outcome of cardiac remodeling under stress conditions. Even though triiodothyronine (T3) has long been recognized as a critical regulator of the cardiac Myh isoform composition, its role as a modulator of the Mhrt/Brg1 axis is still unexplored. Here the effect of T3 on the Mhrt/Brg1 regulatory circuit has been analyzed in relation with chromatin remodeling and previously identified T3-dependent miRNAs. The expression levels of Mhrt, Brg1 and Myh6/Myh7 have been assessed in rat models of hyperthyroidism or acute myocardial ischemia/reperfusion (IR) treated with T3 replacement therapy. To gain mechanistic insights, in silico analyses and site-directed mutagenesis have been adopted in combination with gene reporter assays and loss or gain of function strategies in cultured cardiomyocytes. Our results indicate a pivotal role of Mhrt over-expression in the T3-dependent regulation of Myh switch. Mechanistically, T3 activates the Mhrt promoter at two putative thyroid hormone responsive elements (TRE) located in a crucial region that is necessary for both Mhrt activation and Brg1-dependent Mhrt repression. This newly identified T3 mode of action requires DNA chromatinization and is critically involved in mitigating the repressive function of the Brg1 protein on Mhrt promoter. In addition, T3 is also able to prevent the Brg1 over-expression observed in the post-IR setting through a pathway that might entail the T3-mediated up-regulation of miR-208a. Taken together, our data evidence a novel T3-responsive network of cross-talking epigenetic factors that dictates the cardiac Myh composition and could be of great translational relevance.

    Citation

    Francesca Forini, Giuseppina Nicolini, Claudia Kusmic, Romina D'Aurizio, Alberto Mercatanti, Giorgio Iervasi, Letizia Pitto. T3 Critically Affects the Mhrt/Brg1 Axis to Regulate the Cardiac MHC Switch: Role of an Epigenetic Cross-Talk. Cells. 2020 Sep 24;9(10)

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 32987653

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.