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Initiation of trophectoderm lineage specification in mouse embryos is independent of Cdx2

机译:小鼠胚胎中滋养外胚层谱系规格的启动独立于Cdx2

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摘要

The separation of the first two lineages – trophectoderm (TE) and inner cell mass (ICM) – is a crucial event in the development of the early embryo. The ICM, which constitutes the pluripotent founder cell population, develops into the embryo proper, whereas the TE, which comprises the surrounding outer layer, supports the development of the ICM before and after implantation. Cdx2, the first transcription factor expressed specifically in the developing TE, is crucial for the differentiation of cells into the TE, as lack of zygotic Cdx2 expression leads to a failure of embryos to hatch and implant into the uterus. However, speculation exists as to whether maternal Cdx2 is required for initiation of TE lineage separation. Here, we show that effective elimination of both maternal and zygotic Cdx2 transcripts by an RNA interference approach resulted in failure of embryo hatching and implantation, but the developing blastocysts exhibited normal gross morphology, indicating that TE differentiation had been initiated. Expression of keratin 8, a marker for differentiated TE, further confirmed the identity of the TE lineage in Cdx2-deficient embryos. However, these embryos exhibited low mitochondrial activity and abnormal ultrastructure, indicating that Cdx2 plays a key role in the regulation of TE function. Furthermore, we found that embryonic compaction does not act as a `switch' regulator to turn on Cdx2 expression. Our results clearly demonstrate that neither maternal nor zygotic Cdx2 transcripts direct the initiation of ICM/TE lineage separation.
机译:前两个谱系(滋养外胚层(TE)和内部细胞团(ICM))的分离是早期胚胎发育的关键事件。组成多能基础细胞群的ICM发育成胚胎固有的,而包含周围外层的TE支持植入前后ICM的发育。 Cdx2是在发育中的TE中特异性表达的第一个转录因子,对于细胞向TE的分化至关重要,因为缺乏合子的Cdx2表达会导致胚胎无法孵化并植入子宫。然而,关于是否需要母体Cdx2来启动TE谱系分离的猜测。在这里,我们显示通过RNA干扰方法有效消除母体和合子Cdx2转录物会导致胚胎孵化和植入失败,但是发育中的胚泡表现出正常的总体形态,表明TE分化已经开始。角蛋白8(一种分化的TE的标志物)的表达进一步证实了Cdx2缺陷型胚胎中TE谱系的身份。但是,这些胚胎表现出较低的线粒体活性和异常的超微结构,表明Cdx2在调节TE功能中起关键作用。此外,我们发现胚胎压实不能作为开启Cdx2表达的“开关”调节子。我们的结果清楚地表明,母本和合子Cdx2转录本均未指导ICM / TE谱系分离的启动。

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