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体外受精或体细胞核移植后获得的牛(Bos taurus)胚胎中赖氨酸27位点三甲基化的H3组蛋白的核形态。

Nuclear profiles of H3 histones trimethylated on Lys27 in bovine (Bos taurus) embryos obtained after in vitro fertilization or somatic cell nuclear transfer.

作者信息

Breton Amandine, LE Bourhis Daniel, Audouard Christophe, Vignon Xavier, Lelièvre Jean-Marc

机构信息

INRA, ENVA UMR 1198 Biologie du Développement et Reproduction, France.

出版信息

J Reprod Dev. 2010 Aug;56(4):379-88. doi: 10.1262/jrd.09-182a. Epub 2010 Apr 22.

Abstract

Histone H3 trimethylation on lysine 27 is one of the histone modifications associated with chromatin of silenced regions. H3K27me3 labeling is initially asymmetrical between pronuclei in mammalian embryos, and then it is remodeled during early development. However, in mouse embryos obtained after somatic cell nuclear transfer (SCNT), H3K27me3 histones inherited from the somatic female cell and associated with X chromosome inactivation have been reported to escape remodeling. Using immunostaining, we investigated the remodeling of H3K27me3 in Bos taurus embryos obtained after in vitro fertilization (IVF) and SCNT. In this species, transfer-induced chromatin remodeling can be clearly separated from embryonic genome activation (EGA), which occurs at the 8-16-cell stage, and cloning by SCNT is 10 times more successful than in the mouse. In early IVF bovine embryos, dense H3K27me3 labeling was localized in the pericentric heterochromatin as recently described in the mouse. Labeling was however unevenly distributed up to the 8-cell stage, suggesting that the parental genomes partitioned before EGA. In female IVF blastocysts, a somatic-like female profile appeared in 21% of the trophoblast cells. This profile, which had one major nuclear H3K27me3 patch, the putative inactive X chromosome (Xi), was absent in male blastocysts. In contrast, the somatic-like female H3K27me3 profile was observed in the majority of the nuclei of female bovine SCNT embryos before EGA. At the 8-16-cell stage, this profile was transiently replaced by pericentric-like labeling in most nuclei. Immunostaining of mitotic chromosomes suggested that the ratio of H3K27me3 labeling in pericentric heterochromatin vs. euchromatin was then rapidly altered. Finally, Xi-like H3K27me3 staining appeared again in trophoblast cells in female SCNT blastocysts. These results suggest a role for EGA in H3K27me3 remodeling, which affects the heterochromatin inherited from the donor cell or produced during development.

摘要

赖氨酸27位的组蛋白H3三甲基化是与沉默区域染色质相关的组蛋白修饰之一。在哺乳动物胚胎中,H3K27me3标记最初在原核之间是不对称的,然后在早期发育过程中发生重塑。然而,据报道,在体细胞核移植(SCNT)后获得的小鼠胚胎中,从体雌性细胞继承并与X染色体失活相关的H3K27me3组蛋白逃避了重塑。我们使用免疫染色研究了体外受精(IVF)和SCNT后获得的牛胚胎中H3K27me3的重塑。在这个物种中,转移诱导的染色质重塑可以与胚胎基因组激活(EGA)清楚地分开,EGA发生在8-16细胞阶段,并且通过SCNT进行克隆的成功率比小鼠高10倍。在早期IVF牛胚胎中,密集的H3K27me3标记如最近在小鼠中所描述的那样定位于着丝粒周围异染色质中。然而,在8细胞阶段之前,标记分布不均匀,这表明亲本基因组在EGA之前就进行了分配。在雌性IVF囊胚中,21%的滋养层细胞出现了类似体细胞的雌性特征。这种特征有一个主要的核H3K27me3斑块,即推定的失活X染色体(Xi),在雄性囊胚中不存在。相比之下,在EGA之前,在大多数雌性牛SCNT胚胎的细胞核中观察到了类似体细胞的雌性H3K27me3特征。在8-16细胞阶段,大多数细胞核中的这种特征被类似着丝粒的标记短暂取代。有丝分裂染色体的免疫染色表明,着丝粒周围异染色质与常染色质中H3K27me3标记的比例随后迅速改变。最后,在雌性SCNT囊胚的滋养层细胞中再次出现了类似Xi的H3K27me3染色。这些结果表明EGA在H3K27me3重塑中起作用,这会影响从供体细胞继承或在发育过程中产生的异染色质。

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