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人类胚胎的第一次有丝分裂高度易错。

The first mitotic division of human embryos is highly error prone.

机构信息

Division of Biomedical Sciences, Warwick Medical School, University of Warwick, Coventry, CV4 7AL, UK.

Centre for Mechanochemical Cell Biology, University of Warwick, Coventry, CV4 7AL, UK.

出版信息

Nat Commun. 2022 Nov 8;13(1):6755. doi: 10.1038/s41467-022-34294-6.

Abstract

Human beings are made of ~50 trillion cells which arise from serial mitotic divisions of a single cell - the fertilised egg. Remarkably, the early human embryo is often chromosomally abnormal, and many are mosaic, with the karyotype differing from one cell to another. Mosaicism presumably arises from chromosome segregation errors during the early mitotic divisions, although these events have never been visualised in living human embryos. Here, we establish live cell imaging of chromosome segregation using normally fertilised embryos from an egg-share-to-research programme, as well as embryos deselected during fertility treatment. We reveal that the first mitotic division has an extended prometaphase/metaphase and exhibits phenotypes that can cause nondisjunction. These included multipolar chromosome segregations and lagging chromosomes that lead to formation of micronuclei. Analysis of nuclear number and size provides evidence of equivalent phenotypes in 2-cell human embryos that gave rise to live births. Together this shows that errors in the first mitotic division can be tolerated in human embryos and uncovers cell biological events that contribute to preimplantation mosaicism.

摘要

人类由约 50 万亿个细胞组成,这些细胞来源于单个细胞——受精卵的连续有丝分裂。值得注意的是,早期人类胚胎通常染色体异常,许多是嵌合体,即核型在不同细胞之间存在差异。嵌合体可能是由于早期有丝分裂过程中的染色体分离错误引起的,尽管这些事件从未在活体人类胚胎中被观察到。在这里,我们使用来自卵子共享研究计划的正常受精胚胎以及在生育治疗中被淘汰的胚胎,建立了染色体分离的活细胞成像。我们揭示了第一次有丝分裂具有延长的前期/中期,并表现出可能导致非整倍体的表型。这些表型包括多极染色体分离和滞后染色体,导致微核形成。核数和大小的分析为导致活产的 2 细胞人类胚胎的等效表型提供了证据。综上所述,这表明第一次有丝分裂中的错误可以在人类胚胎中被容忍,并揭示了导致胚胎前嵌合体的细胞生物学事件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/43f9/9643329/1b82cab20009/41467_2022_34294_Fig1_HTML.jpg

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