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从精子到着床阶段父本基因组中父本表达基因上H3K4me3的存在情况。

Presence of H3K4me3 on Paternally Expressed Genes of the Paternal Genome From Sperm to Implantation.

作者信息

Ishihara Teruhito, Griffith Oliver W, Suzuki Shunsuke, Renfree Marilyn B

机构信息

School of BioSciences, The University of Melbourne, Melbourne, VIC, Australia.

Department of Biological Sciences, Macquarie University, Sydney, NSW, Australia.

出版信息

Front Cell Dev Biol. 2022 Mar 10;10:838684. doi: 10.3389/fcell.2022.838684. eCollection 2022.

Abstract

Genomic imprinting, parent-of-origin-specific gene expression, is controlled by differential epigenetic status of the parental chromosomes. While DNA methylation and suppressive histone modifications established during gametogenesis suppress imprinted genes on the inactive allele, how and when the expressed allele gains its active status is not clear. In this study, we asked whether the active histone-3 lysine-4 trimethylation (H3K4me3) marks remain at paternally expressed genes (PEGs) in sperm and embryos before and after fertilization using published data. Here we show that mouse sperm had the active H3K4me3 at more than half of known PEGs, and these genes were present even after fertilization. Using reciprocal cross data, we identified 13 new transient PEGs during zygotic genome activation. Next, we confirmed that the 12 out of the 13 new transient PEGs were associated with the paternal H3K4me3 in sperm. Nine out of the 12 genes were associated with the paternal H3K4me3 in zygotes. Our results show that paternal H3K4me3 marks escape inactivation during the histone-to-protamine transition that occurs during sperm maturation and are present in embryos from early zygotic stages up to implantation.

摘要

基因组印记,即亲本来源特异性基因表达,受亲本染色体不同表观遗传状态的控制。虽然配子发生过程中建立的DNA甲基化和抑制性组蛋白修饰会抑制非活性等位基因上的印记基因,但表达的等位基因如何以及何时获得其活性状态尚不清楚。在本研究中,我们利用已发表的数据,探究了在受精前后,精子和胚胎中父本表达基因(PEGs)上的活性组蛋白H3赖氨酸4三甲基化(H3K4me3)标记是否仍然存在。我们发现,小鼠精子中超过一半的已知PEGs具有活性H3K4me3标记,且这些基因在受精后依然存在。利用正反交数据,我们在合子基因组激活过程中鉴定出13个新的瞬时PEGs。接下来,我们证实了这13个新的瞬时PEGs中有12个与精子中的父本H3K4me3相关。这12个基因中有9个与合子中的父本H3K4me3相关。我们的结果表明,父本H3K4me3标记在精子成熟过程中发生的组蛋白向鱼精蛋白转变期间逃避了失活,并在从合子早期到着床的胚胎中存在。

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