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首页> 外文期刊>Genesis: the journal of genetics and development >Cre-conditional expression of constitutively active Notch1 in transgenic mice.
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Cre-conditional expression of constitutively active Notch1 in transgenic mice.

机译:组成性活性Notch1在转基因小鼠中的cre条件表达。

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摘要

The Notch signaling pathway plays a critical role during mammalian development. To bypass embryonic lethality associated with constitutive Notch1 signaling, we created transgenic mice with a floxed beta-geo/stop signal between a cytomegalo virus promoter and the constitutively active intracellular domain of Notch1 (IC-Notch1). IC-Notch1 is activated upon introduction of Cre recombinase and it is coexpressed with an enhanced green fluorescent protein or human placental alkaline phosphatase reporter. We created three IC-Notch1 transgenic mouse lines and crossed them to a general Cre deletor mouse line, pCX-Cre. The double transgenic IC-Notch1/pCX-Cre embryos have widespread expression of IC-Notch1 and reporters and die before 10.5 days of gestation. Morphological and histological analysis of the double transgenic embryos indicated growth arrest and various developmental defects, including lack of neural tube closure, disorganized somites, and disrupted vasculature. The conditional IC-Notch1 expressing transgenic mice provide a unique tool to investigate the Notch pathway using tissue-specific Cre mice and inducible Cre systems.
机译:Notch信号通路在哺乳动物发育过程中起着至关重要的作用。为了绕过与组成性Notch1信号传导相关的胚胎致死力,我们创建了转基因小鼠,其巨细胞病毒启动子与Notch1的组成型活性细胞内结构域(IC-Notch1)之间具有模糊的be​​ta-geo / stop信号。 IC-Notch1在引入Cre重组酶后被激活,并与增强的绿色荧光蛋白或人胎盘碱性磷酸酶报道分子共表达。我们创建了三个IC-Notch1转基因小鼠品系,并将它们与通用的Cre删除子小鼠品系pCX-Cre杂交。双转基因IC-Notch1 / pCX-Cre胚胎具有IC-Notch1和报告基因的广泛表达,并在妊娠10.5天之前死亡。对双转基因胚胎的形态学和组织学分析表明,生长停滞和各种发育缺陷,包括缺乏神经管闭合,无节理的体节和脉管系统破裂。表达条件性IC-Notch1的转基因小鼠提供了独特的工具,可使用组织特异性Cre小鼠和可诱导的Cre系统研究Notch途径。

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