Wt1 transcription factor impairs cardiomyocyte specification and drives a phenotypic switch from myocardium to epicardium
Author(s) -
Inês J. Marques,
Alexander Ernst,
Prateek Arora,
Andréj Vianin,
Tanja Hetke,
Andrés Sanz-Morejón,
Uta Naumann,
Adolfo Odriozola,
Xavier Langa,
Laura AndrésDelgado,
Benoît Zuber,
Carlos Torroja,
Marco Osterwalder,
Filipa C. Simões,
Christoph Englert,
Nadia Mercader
Publication year - 2022
Publication title -
development
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.754
H-Index - 325
eISSN - 1477-9129
pISSN - 0950-1991
DOI - 10.1242/dev.200375
Subject(s) - biology , transdifferentiation , mef2c , microbiology and biotechnology , pericardium , myocyte , ectopic expression , transcription factor , progenitor cell , zebrafish , mef2 , heart development , intercalated disc , anatomy , gene , medicine , stem cell , enhancer , embryonic stem cell , genetics , gap junction , intracellular
During development, the heart grows by addition of progenitor cells to the poles of the primordial heart tube. In the zebrafish, Wilms tumor 1 transcription factor a (wt1a) and b (wt1b) genes are expressed in the pericardium, at the venous pole of the heart. From this pericardial layer, the proepicardium emerges. Proepicardial cells are subsequently transferred to the myocardial surface and form the epicardium, covering the myocardium. We found that while wt1a and wt1b expression is maintained in proepicardial cells, it is downregulated in pericardial cells that contributes cardiomyocytes to the developing heart. Sustained wt1b expression in cardiomyocytes reduced chromatin accessibility of specific genomic loci. Strikingly, a subset of wt1a- and wt1b-expressing cardiomyocytes changed their cell-adhesion properties, delaminated from the myocardium and upregulated epicardial gene expression. Thus, wt1a and wt1b act as a break for cardiomyocyte differentiation, and ectopic wt1a and wt1b expression in cardiomyocytes can lead to their transdifferentiation into epicardial-like cells.
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