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EndoG is dispensable in embryogenesis and apoptosis.

机译:EndoG在胚胎发生和凋亡中是必不可少的。

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The mitochondrial protein, endonuclease G (EndoG), is one of the endonucleases implicated in DNA fragmentation during apoptosis. It has been shown to translocate from the mitochondria to the nucleus upon cell death stimuli. These observations suggest that EndoG is a mitochondrial cell death effector, and that it possibly acts as a cell death nuclease, similar to DNA fragmentation factor. To better understand the role of EndoG in development and apoptosis, we generated EndoG null mice by homologous gene targeting without disruption of D2Wsu81e. EndoG null mice are viable and develop to adulthood with no obvious abnormalities. Fibroblasts generated from the EndoG null mice show no difference in susceptibility when induced to die by a variety of intrinsic and extrinsic apoptotic stimuli. Additionally, EndoG null mice are equally sensitive to excitotoxic stress. These data suggest that EndoG is not essential for early embryogenesis and apoptosis.
机译:线粒体蛋白内切核酸酶G(EndoG)是细胞凋亡过程中与DNA片段化有关的内切核酸酶之一。已经表明,在细胞死亡刺激后,它可以从线粒体转移到细胞核。这些观察结果表明,EndoG是线粒体细胞死亡的效应器,它可能起细胞死亡核酸酶的作用,类似于DNA断裂因子。为了更好地了解EndoG在发育和凋亡中的作用,我们通过不破坏D2Wsu81e的同源基因靶向生成了EndoG null小鼠。 EndoG无效小鼠存活并发展到成年,无明显异常。从EndoG null小鼠产生的成纤维细胞在被多种内在和外在的凋亡刺激诱导死亡时,在磁化率上没有差异。此外,EndoG null小鼠对兴奋性毒性应激同样敏感。这些数据表明EndoG对于早期胚胎发生和凋亡不是必需的。

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