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NKX2-5 regulates human cardiomyogenesis via a HEY2 dependent transcriptional network.

Nat Commun. 2018; 
Anderson DJ, Kaplan DI, Bell KM, Koutsis K, Haynes JM, Mills RJ, Phelan DG, Qian EL, Leitoguinho AR, Arasaratnam D, Labonne T, Ng ES, Davis RP, Casini S, Passier R, Hudson JE, Porrello ER, Costa MW, Rafii A,, Curl CL, Delbridge LM, Harvey RP,, Oshlack A, Cheung MM,, Mummery CL, Petrou S, Elefanty AG,,, Stanley EG,,, Elliott DA,,.
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Custom Vector Construction The NKX2-5 expression vector was purchased from GenScript (pcDNA3. Get A Quote

摘要

Congenital heart defects can be caused by mutations in genes that guide cardiac lineage formation. Here, we show deletion of NKX2-5, a critical component of the cardiac gene regulatory network, in human embryonic stem cells (hESCs), results in impaired cardiomyogenesis, failure to activate VCAM1 and to downregulate the progenitor marker PDGFRα. Furthermore, NKX2-5 null cardiomyocytes have abnormal physiology, with asynchronous contractions and altered action potentials. Molecular profiling and genetic rescue experiments demonstrate that the bHLH protein HEY2 is a key mediator of NKX2-5 function during human cardiomyogenesis. These findings identify HEY2 as a novel component of the NKX2-5 cardiac transcriptiona... More

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