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In vivo detection of programmed cell death during mouse heart development

机译:在小鼠心脏发育过程中的体内检测程序化细胞死亡

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Despite the great progress on the cell biology of programmed cell death (PCD), its incidence and exact time course during embryonic and particular heart development are still unclear. This is also due to the lack of models enabling to directly identify and monitor PCD cells at different time points in vivo. Herein we report generation of transgenic murine embryonic stem cell and mouse models expressing secreted Annexin V-YFP under control of the CAG promoter. This enables to visualize and quantify PCD in vitro and in vivo during embryonic development. At early embryonic stages we found Annexin V-YFP+ fluorescent cells in known areas of PCD, such as the otic ring and at the site of neural tube closing, underscoring its specificity for detection of PCD. We have focused our detailed analysis primarily on PCD in the embryonic heart for a better understanding of its role during development. Our findings reveal that PCD peaks at early stages of cardiogenesis (E9.5-E13.5) and strongly decreases thereafter. Moreover, the PCD cells in the heart are predominantly cardiomyocytes, and an unexpected area of prominent cardiac PCD are the ventricular trabeculae (E9.5-E14.5). Thus, the sA5-YFP mouse line provides novel insight into the incidence and relevance of cardiac PCD during embryonic development ex- and in vivo.
机译:尽管对编程细胞死亡(PCD)的细胞生物学进行了巨大进展,但其在胚胎和特殊心脏发育期间的发病率和精确时间过程仍然不清楚。这也是由于缺乏在体内不同时间点直接识别和监控PCD细胞的模型。在此,我们在CAG启动子的控制下报告了表达分泌的膜蛋白V-YFP的转基因鼠胚胎干细胞和小鼠模型。这使得能够在胚胎发育期间在体外和体内进行可视化和量化PCD。在早期胚胎阶段,我们发现了PCD的已知区域中的膜蛋白V-YFP +荧光细胞,例如耳环和神经管关闭部位,强调其对PCD检测的特异性。我们主要专注于胚胎心脏在PCD上的详细分析,以更好地了解其在开发期间的作用。我们的研究结果表明,心肌发生的早期阶段的PCD峰(E9.5-E13.5),此后强烈降低。此外,心脏中的PCD细胞主要是心肌细胞,并且突出的心脏PCD的意外区域是心室组织(E9.5-E14.5)。因此,SA5-YFP鼠标系列提供了对心脏PCD在胚胎发育期间和体内胚胎发育期间的发病率和相关性的新颖性。

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