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非整倍体和 DNA 甲基化作为早期人类胚胎发育的镜像特征。

Aneuploidy and DNA Methylation as Mirrored Features of Early Human Embryo Development.

机构信息

Research Institute of Medical Genetics, Tomsk National Research Medical Center, 634050 Tomsk, Russia.

出版信息

Genes (Basel). 2020 Sep 17;11(9):1084. doi: 10.3390/genes11091084.

Abstract

Genome stability is an integral feature of all living organisms. Aneuploidy is the most common cause of fetal death in humans. The timing of bursts in increased aneuploidy frequency coincides with the waves of global epigenetic reprogramming in mammals. During gametogenesis and early embryogenesis, parental genomes undergo two waves of DNA methylation reprogramming. Failure of these processes can critically affect genome stability, including chromosome segregation during cell division. Abnormal methylation due to errors in the reprogramming process can potentially lead to aneuploidy. On the other hand, the presence of an entire additional chromosome, or chromosome loss, can affect the global genome methylation level. The associations of these two phenomena are well studied in the context of carcinogenesis, but here, we consider the relationship of DNA methylation and aneuploidy in early human and mammalian ontogenesis. In this review, we link these two phenomena and highlight the critical ontogenesis periods and genome regions that play a significant role in human reproduction and in the formation of pathological phenotypes in newborns with chromosomal aneuploidy.

摘要

基因组稳定性是所有生物的基本特征。非整倍体是人类胎儿死亡的最常见原因。非整倍体频率增加的爆发时间与哺乳动物中全球表观遗传重编程的波动相吻合。在配子发生和早期胚胎发生过程中,亲代基因组经历了两次 DNA 甲基化重编程的浪潮。这些过程的失败会严重影响基因组稳定性,包括细胞分裂过程中的染色体分离。由于重编程过程中的错误导致的异常甲基化可能导致非整倍体。另一方面,整条额外染色体的存在或染色体缺失会影响全球基因组甲基化水平。这两种现象的关联在致癌作用的背景下得到了很好的研究,但在这里,我们考虑了 DNA 甲基化与人类和哺乳动物个体发生早期非整倍体的关系。在这篇综述中,我们将这两种现象联系起来,并强调了在人类生殖和具有染色体非整倍体的新生儿病理性表型形成中起重要作用的关键个体发生期和基因组区域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c37c/7564410/1e78ff5839a9/genes-11-01084-g001.jpg

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