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首页> 外文期刊>Genome research >Cell fate inclination within 2-cell and 4-cell mouse embryos revealed by single-cell RNA sequencing.
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Cell fate inclination within 2-cell and 4-cell mouse embryos revealed by single-cell RNA sequencing.

机译:单细胞RNA测序揭示了2细胞和4细胞小鼠胚胎中的细胞命运倾向。

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摘要

It remains an open question when and how the first cell fate decision is made in mammals. Using deep single-cell RNA-seq of matched sister blastomeres, we report highly reproducible inter-blastomere differences among 10 2-cell and five 4-cell mouse embryos. Inter-blastomere gene expression differences dominated between-embryo differences and noise, and were sufficient to cluster sister blastomeres into distinct groups. Dozens of protein-coding genes exhibited reproducible bimodal expression in sister blastomeres, which cannot be explained by random fluctuations. The protein expression of one gene out of four of these bimodal genes tested, Gadd45a, exhibited clear inter-blastomeric contrasts. We traced some of the bimodal mRNA expressions to embryonic genome activation, and others to blastomere-specific RNA depletion. Inter-blastomere differences created coexpression gene networks that were much stronger and larger than those that can possibly be created by random noise. The highly correlated gene pairs at the 4-cell stage overlapped with those showing the same directions of differential expression between inner cell mass (ICM) and trophectoderm (TE). These data substantiate the hypothesis of inter-blastomere differences in 2- and 4-cell mouse embryos, and associate these differences with ICM/TE differences.
机译:何时以及如何在哺乳动物中做出第一个细胞命运决定仍然是一个悬而未决的问题。使用匹配的姐妹卵裂球的深层单细胞RNA-seq,我们报道了10个2细胞和5个4细胞小鼠胚胎之间的高可重复性卵裂球差异。卵裂球间基因表达差异主导着胚间差异和噪音,足以将姐妹卵裂球聚类为不同的群体。数十个蛋白质编码基因在姐妹卵裂球中表现出可再现的双峰表达,这不能用随机波动来解释。测试的这些双峰基因中的四个基因中的一个基因(Gadd45a)的蛋白质表达表现出明显的胚泡间差异。我们追踪到双峰mRNA表达的某些胚胎基因组激活,和其他的卵裂球特定RNA消耗。卵裂球间的差异产生了共表达基因网络,该网络比可能由随机噪声产生的共表达基因网络要强大得多。在4细胞阶段高度相关的基因对与那些显示内部细胞团(ICM)和滋养外胚层(TE)之间差异表达方向相同的基因对重叠。这些数据证实了2细胞和4细胞小鼠胚胎中卵裂球间差异的假设,并将这些差异与ICM / TE差异相关联。

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