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2 细胞期小鼠胚胎中卵裂球全能性的差异是一种母源性特征,由不对称的 mRNA 分布介导。

Differences in blastomere totipotency in 2-cell mouse embryos are a maternal trait mediated by asymmetric mRNA distribution.

机构信息

Max Planck Institute for Molecular Biomedicine, Muenster, Germany.

Core Genomic Facility, University Hospital Muenster, Muenster, Germany.

出版信息

Mol Hum Reprod. 2019 Nov 30;25(11):729-744. doi: 10.1093/molehr/gaz051.

Abstract

It is widely held that the first two blastomeres of mammalian embryos are equally totipotent and that this totipotency belongs to the group of regulative properties. However, this interpretation neglects an important aspect: evidence only came from successful monozygotic twins which can speak only for those pairs of half-embryos that are able to regulate in the first place. Are the frequently occurring incomplete pairs simply an artefact, or do they represent a real difference, be it in the imperfect blastomere's ability to regulate growth or in the distribution of any compound X that constrains regulation? Using the model system of mouse embryos bisected at the 2-cell stage after fertilization, we present evidence that the interblastomere differences evade regulation by external factors and are already latent in oocytes. Specifically, an interblastomere imbalance of epiblast production persists under the most diverse culture conditions and applies to the same extent in parthenogenetic counterparts. As a result, cases in which twin blastocysts continued to develop in only one member account for 65 and 57% of zygotic and parthenogenetic pairs, respectively. The interblastomere imbalance is related to the subcellular distribution of gene products, as documented for the epiblast-related gene Cops3, using mRNA FISH in super-resolution mode confocal microscopy. Blastomere patterns of Cops3 mRNA distribution are α-amanitin-resistant. Thus, the imbalance originates not from de novo transcription, but from influences which are effective before fertilisation. These data expose previously unrecognized limits of regulative capacities of 2-cell stage blastomeres and point to aspects of cytoplasmic organization of the mouse oocyte that segregate unequally to blastomeres during cleavage.

摘要

人们普遍认为哺乳动物胚胎的前两个卵裂球具有同等的全能性,这种全能性属于调节性质。然而,这种解释忽略了一个重要方面:证据仅来自成功的单卵双胞胎,这只能说明那些首先能够调节的半胚胎对。经常出现的不完全对是否仅仅是一种假象,或者它们代表了一种真正的差异,无论是在不完善的卵裂球调节生长的能力上,还是在任何限制调节的化合物 X 的分布上?我们使用受精后在 2 细胞阶段将小鼠胚胎二等分的模型系统,提供了证据表明卵裂球之间的差异逃避了外部因素的调节,并且在卵母细胞中已经潜伏。具体来说,在外胚层产生方面,卵裂球之间的不平衡持续存在于最各种培养条件下,并在程度上适用于同卵性双胞胎。因此,在只有一个成员中继续发育的双胞胎囊胚的情况下,占合子和孤雌生殖对的 65%和 57%。卵裂球之间的不平衡与基因产物的亚细胞分布有关,如使用 mRNA FISH 在超分辨率共聚焦显微镜中记录的与外胚层相关的基因 Cops3。Cops3 mRNA 分布的卵裂球模式对α-鹅膏蕈碱具有抗性。因此,不平衡不是来自新转录,而是来自受精前有效的影响。这些数据揭示了 2 细胞阶段卵裂球的调节能力以前未被认识到的限制,并指出了小鼠卵母细胞细胞质组织的方面,在卵裂过程中不均匀地分配给卵裂球。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e173/6884417/925886a983b5/gaz051f1.jpg

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