標題: Zebrafish VCAP1X2 regulates cardiac contractility and proliferation of cardiomyocytes and epicardial cells
作者: Hsieh, Fang-Chi
Lu, Yu-Fen
Liau, Ian
Chen, Chien-Chang
Cheng, Chao-Min
Hsiao, Chung-Der
Hwang, Sheng-Ping L.
應用化學系
應用化學系分子科學碩博班
Department of Applied Chemistry
Institute of Molecular science
公開日期: 18-五月-2018
摘要: Sarcomeric signaling complexes are important to sustain proper sarcomere structure and function, however, the mechanisms underlying these processes are not fully elucidated. In a gene trap experiment, we found that vascular cell adhesion protein 1 isoform X2 (VCAP1X2) mutant embryos displayed a dilated cardiomyopathy phenotype, including reduced cardiac contractility, enlarged ventricular chamber and thinned ventricular compact layer. Cardiomyocyte and epicardial cell proliferation was decreased in the mutant heart ventricle, as was the expression of pAKT and pERK. Contractile dysfunction in the mutant was caused by sarcomeric disorganization, including sparse myofilament, blurred Z-disc, and decreased gene expression for sarcomere modulators (smyd1b, mypn and fhl2 alpha), sarcomeric proteins (myh6, myh7, vmhcl and tnnt2 alpha) and calcium regulators (ryr2b and slc8a1 alpha). Treatment of PI3K activator restored Z-disc alignment while injection of smyd1b mRNA restored Z-disc alignment, contractile function and cardiomyocyte proliferation in ventricles of VCAP1X2 mutant embryos. Furthermore, injection of VCAP1X2 variant mRNA rescued all phenotypes, so long as two cytosolic tyrosines were left intact. Our results reveal two tyrosine residues located in the VCAP1X2 cytoplasmic domain are essential to regulate cardiac contractility and the proliferation of ventricular cardiomyocytes and epicardial cells through modulating pAKT and pERK expression levels.
URI: http://dx.doi.org/10.1038/s41598-018-26110-3
http://hdl.handle.net/11536/145000
ISSN: 2045-2322
DOI: 10.1038/s41598-018-26110-3
期刊: SCIENTIFIC REPORTS
Volume: 8
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