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两种组蛋白甲基转移酶在. 中跨代传递基于 H3K36me3 的表观遗传记忆中的独特作用

Distinct Roles of Two Histone Methyltransferases in Transmitting H3K36me3-Based Epigenetic Memory Across Generations in .

机构信息

Department of Molecular, Cell and Developmental Biology, University of California Santa Cruz, Santa Cruz, California 95064.

Epigenetics Institute, Department of Biochemistry and Biophysics, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104.

出版信息

Genetics. 2018 Nov;210(3):969-982. doi: 10.1534/genetics.118.301353. Epub 2018 Sep 14.

Abstract

Epigenetic information contributes to proper gene expression and development, and can be transmitted not only through mitotic divisions but also from parents to progeny. We investigated the roles in epigenetic inheritance of MES-4 and MET-1, the two enzymes that methylate H3K36 (histone H3 Lys 36). Mass spectrometry analysis confirmed immunostaining results showing that both MES-4 and MET-1 catalyze H3K36me3. In the adult germline, MES-4 is enriched in the distal mitotic zone and MET-1 is enriched in the meiotic pachytene zone. Embryos inherit H3K36me3-marked chromosomes from both the oocyte and sperm, and a maternal load of MES-4 and MET-1 Maternal MES-4 quickly associates with sperm chromosomes; that association requires that the sperm chromosomes bear H3K36me3, suggesting that MES-4 is recruited to chromosomes by preexisting H3K36me3. In embryos that inherit H3K36me3-positive oocyte chromosomes and H3K36me3-negative sperm chromosomes, MES-4 and H3K36me3 are maintained on only a subset of chromosomes until at least the 32-cell stage, likely because MES-4 propagates H3K36me3 on regions of the genome with preexisting H3K36me3. In embryos lacking MES-4, H3K36me3 levels on chromosomes drop precipitously postfertilization. In contrast to the relatively high levels of MES-4 in early-stage embryos, MET-1 levels are low at early stages and start increasing by the ∼26-cell stage, consistent with expression from the zygotic genome. Our findings support the model that MET-1 mediates transcription-coupled H3K36me3 in the parental germline and transcriptionally active embryos, and that MES-4 transmits an epigenetic memory of H3K36me3 across generations and through early embryo cell divisions by maintaining inherited patterns of H3K36me3.

摘要

表观遗传信息有助于基因的正确表达和发育,并且可以通过有丝分裂分裂传递,也可以从父母传递给后代。我们研究了两个酶 MES-4 和 MET-1 在表观遗传遗传中的作用,这两个酶将 H3K36(组蛋白 H3 赖氨酸 36)甲基化。质谱分析结果证实了免疫染色结果,表明 MES-4 和 MET-1 都催化 H3K36me3。在成体生殖细胞中,MES-4 在远端有丝分裂区富集,MET-1 在减数分裂粗线期区富集。胚胎从卵子和精子中继承 H3K36me3 标记的染色体,MES-4 和 MET-1 的母体负荷迅速与精子染色体结合;这种结合需要精子染色体带有 H3K36me3,表明 MES-4 通过预先存在的 H3K36me3 被招募到染色体上。在从卵子继承 H3K36me3 阳性染色体而从精子继承 H3K36me3 阴性染色体的胚胎中,MES-4 和 H3K36me3 仅在至少 32 细胞阶段之前维持在一组染色体上,这可能是因为 MES-4 在基因组中具有预先存在的 H3K36me3 的区域上传播 H3K36me3。在缺乏 MES-4 的胚胎中,受精后染色体上的 H3K36me3 水平急剧下降。与早期胚胎中相对较高的 MES-4 水平相比,MET-1 的水平在早期阶段较低,并且从大约 26 细胞阶段开始增加,与合子基因组的表达一致。我们的研究结果支持这样的模型,即 MET-1 介导亲代生殖细胞和转录活性胚胎中与转录偶联的 H3K36me3,而 MES-4 通过维持 H3K36me3 的遗传模式,在代际之间和早期胚胎细胞分裂中传递 H3K36me3 的表观遗传记忆。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a5ec/6218224/a09f5bd11bcf/969fig1.jpg

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