Goodman Cancer Research Centre, Department of Human Genetics, McGill University, 1160 Pine Avenue West, Rm 419, Canada.
Dev Biol. 2013 Dec 1;384(1):65-71. doi: 10.1016/j.ydbio.2013.09.023. Epub 2013 Sep 21.
The primitive endoderm (PE) and epiblast (EPI) are two lineages derived from the inner cell mass (ICM) of the E3.5 blastocyst. Although it has been shown that FGF signaling is necessary and sufficient for PE specification in the ICM, it is unknown what mechanisms control the PE/EPI proportion in the embryo. Because modulation of FGF signaling alone is sufficient to convert all ICM cells to either PE or EPI, a model has been proposed in which the amount of FGF in the embryo controls the PE/EPI proportion. To test this model, we reduced the amount of FGF4, the major FGF in the preimplantation embryo, using various genotypes of Fgf4 mutants. We observed a maternal contribution of Fgf4 in PE specification, but it was dispensable for development. In addition, upon treatment of Fgf4 mutant embryos with exogenous FGF4, we observed a progressive increase of PE proportions in an FGF4 dose dependent manner, regardless of embryo genotype. We conclude that the amount of FGF4 is limited and regulates PE/EPI proportions in the mouse embryo.
原始内胚层 (PE) 和上胚层 (EPI) 是从 E3.5 囊胚的内细胞团 (ICM) 中衍生出来的两个谱系。尽管已经表明 FGF 信号对于 ICM 中 PE 特化是必需且充分的,但尚不清楚什么机制控制胚胎中 PE/EPI 的比例。因为单独调节 FGF 信号足以将所有 ICM 细胞转化为 PE 或 EPI,因此提出了一个模型,即胚胎中 FGF 的数量控制着 PE/EPI 的比例。为了验证该模型,我们使用各种 Fgf4 突变体的基因型来减少主要存在于植入前胚胎中的 FGF4 的量。我们观察到母源 Fgf4 在 PE 特化中的作用,但它对发育是可有可无的。此外,在用外源性 FGF4 处理 Fgf4 突变体胚胎时,我们观察到无论胚胎基因型如何,PE 比例都以 FGF4 剂量依赖性的方式逐渐增加。我们得出结论,FGF4 的量是有限的,并调节着小鼠胚胎中 PE/EPI 的比例。
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