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Publication : HIC2 regulates isoform switching during maturation of the cardiovascular system.

First Author  Dykes IM Year  2018
Journal  J Mol Cell Cardiol Volume  114
Pages  29-37 PubMed ID  29061339
Mgi Jnum  J:257501 Mgi Id  MGI:6115093
Doi  10.1016/j.yjmcc.2017.10.007 Citation  Dykes IM, et al. (2018) HIC2 regulates isoform switching during maturation of the cardiovascular system. J Mol Cell Cardiol 114:29-37
abstractText  Physiological changes during embryonic development are associated with changes in the isoform expression of both myocyte sarcomeric proteins and of erythrocyte haemoglobins. Cell type-specific isoform expression of these genes also occurs. Although these changes appear to be coordinated, it is unclear how changes in these disparate cell types may be linked. The transcription factor Hic2 is required for normal cardiac development and the mutant is embryonic lethal. Hic2 embryos exhibit precocious expression of the definitive-lineage haemoglobin Hbb-bt in circulating primitive erythrocytes and of foetal isoforms of cardiomyocyte genes (creatine kinase, Ckm, and eukaryotic elongation factor Eef1a2) as well as ectopic cardiac expression of fast-twitch skeletal muscle troponin isoforms. We propose that HIC2 regulates a switching event within both the contractile machinery of cardiomyocytes and the oxygen carrying systems during the developmental period where demands on cardiac loading change rapidly.
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