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Enhanced cardiogenesis in embryonic stem cells overexpressing the GATA-4 transcription factor.

机译:过度表达GATA-4转录因子的胚胎干细胞中增强的心脏发生。

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GATA-4 is a cardiac-specific member of the GATA family of zinc finger transcription factors. During embryogenesis, GATA-4 expression is detected very early in the cardiogenic area and persists later in the developing heart. Studies have shown that GATA-4 is a potent transcriptional activator of several cardiac muscle-specific genes and a key regulator of the cardiomyocyte gene program. Consistent with a role for GATA-4 in cardiomyocyte formation, inhibition of GATA-4 expression by antisense transcripts interferes with expression of cardiac muscle genes and blocks development of beating cardiomyocytes in P19 embryonic stem cells. In order to better define the function of GATA-4 in cardiogenesis, we have carried out molecular analysis of early stages of cardiomyocyte differentiation in GATA-4-deficient P19 cell lines and in P19 cells stably overexpressing GATA-4. The results indicate that GATA-4 is not required for either endodermal or mesodermal commitment or for initiation of the cardiac pathway. However, in the absence of GATA-4, differentiation is blocked at the precardiac (cardioblasts) stage and cells are lost through extensive apoptosis. In contrast, ectopic expression of GATA-4 in P19 cells accelerates cardiogenesis and markedly increases (over 10-fold) the number of terminally differentiated beating cardiomyocytes following cell aggregation. Together, these findings suggest that, in addition to its role in activation of the cardiac genetic program, GATA-4 may be the nuclear target of inductive and/or survival factors for precardiac cells.
机译:GATA-4是锌指转录因子GATA家族的心脏特异性成员。在胚胎发生过程中,很早就在心源区检测到了GATA-4表达,并在发育中的心脏中持续存在。研究表明,GATA-4是几种心肌特异性基因的有效转录激活因子,是心肌细胞基因程序的关键调控因子。与GATA-4在心肌细胞形成中的作用一致,反义转录本对GATA-4表达的抑制会干扰心肌基因的表达并阻止P19胚胎干细胞中跳动的心肌细胞的发育。为了更好地定义GATA-4在心脏发生中的功能,我们对GATA-4缺陷的P19细胞系和稳定表达GATA-4的P19细胞进行了心肌细胞分化早期阶段的分子分析。结果表明,GATA-4不需要用于内胚层或中胚层定位,也不需要启动心脏通路。然而,在没有GATA-4的情况下,分化在心前期(成胚细胞)阶段受阻,细胞通过广泛的凋亡而丢失。相反,P19细胞中GATA-4的异位表达加速了心脏发生,并在细胞聚集后显着增加(超过10倍)最终分化的跳动心肌细胞的数量。总之,这些发现表明,除了其在激活心脏遗传程序中的作用外,GATA-4可能是心脏前细胞诱导和/或存活因子的核靶标。

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