| Literature DB >> 26547215 |
Agnese Re1, Simona Nanni2, Aurora Aiello1, Serena Granata2, Claudia Colussi1, Giulia Campostrini3, Francesco Spallotta4, Stefania Mattiussi1, Valentina Pantisano2, Carmen D'Angelo5, Annamaria Biroccio5, Alessandra Rossini6,7, Andrea Barbuti3, Dario DiFrancesco3, Francesco Trimarchi8, Alfredo Pontecorvi2, Carlo Gaetano9, Antonella Farsetti10,11.
Abstract
The epigenetics of early commitment to embryonal cardiomyocyte is poorly understood. In this work, we compared the effect of thyroid hormone and that of anacardic acid, a naturally occurring histone acetylase inhibitor, or both in combination, on mouse embryonic stem cells (mES) differentiating into embryonal cardiomyocyte by embryoid bodies (EBs) formation. Although the results indicated that anacardic acid (AA) and thyroid hormone were both efficient in promoting cardiomyocyte differentiation, we noticed that a transient exposure of mES to AA alone was sufficient to enlarge the beating areas of EBs compared to those of untreated controls. This effect was associated with changes in the chromatin structure at the promoters of specific cardiomyogenic genes. Among them, a rapid induction of the transcription factor Castor 1 (CASZ1), important for cardiomyocytes differentiation and maturation during embryonic development, was observed in the presence of AA. In contrast, thyroid hormone (T 3) was more effective in stimulating spontaneous firing, thus suggesting a role in the production of a population of cardiomyocyte with pacemaker properties. In conclusion, AA and thyroid hormone both enhanced cardiomyocyte formation along in apparently distinct pathways.Entities:
Keywords: Cardiomyocytes; Epigenetics; Lysine acetylation; Mesoderm; Mouse ES
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Year: 2015 PMID: 26547215 DOI: 10.1007/s12020-015-0751-2
Source DB: PubMed Journal: Endocrine ISSN: 1355-008X Impact factor: 3.633