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通过 CRISPR/Cas9 筛选在单倍体人胚胎干细胞中鉴定亲本印迹的调控因子。

Identifying regulators of parental imprinting by CRISPR/Cas9 screening in haploid human embryonic stem cells.

机构信息

The Azrieli Center for Stem Cells and Genetic Research, Department of Genetics, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Edmond J. Safra Campus, Givat Ram, Jerusalem, 91904, Israel.

Department of Genetics, The Alexander Silberman Institute of Life Sciences, The Hebrew University of Jerusalem, Edmond J. Safra Campus, Givat Ram, Jerusalem, 91904, Israel.

出版信息

Nat Commun. 2021 Nov 18;12(1):6718. doi: 10.1038/s41467-021-26949-7.

Abstract

In mammals, imprinted genes are regulated by differentially methylated regions (DMRs) that are inherited from germ cells, leading to monoallelic expression in accordance with parent-of-origin. Yet, it is largely unknown how imprinted DMRs are maintained in human embryos despite global DNA demethylation following fertilization. Here, we explored the mechanisms involved in imprinting regulation by employing human parthenogenetic embryonic stem cells (hpESCs), which lack paternal alleles. We show that although global loss of DNA methylation in hpESCs affects most imprinted DMRs, many paternally-expressed genes (PEGs) remain repressed. To search for factors regulating PEGs, we performed a genome-wide CRISPR/Cas9 screen in haploid hpESCs. This revealed ATF7IP as an essential repressor of a set of PEGs, which we further show is also required for silencing sperm-specific genes. Our study reinforces an important role for histone modifications in regulating imprinted genes and suggests a link between parental imprinting and germ cell identity.

摘要

在哺乳动物中,印迹基因受来自生殖细胞的差异甲基化区域 (DMR) 调控,导致根据亲本来源的单等位基因表达。然而,尽管受精后基因组 DNA 去甲基化,印迹 DMR 如何在人类胚胎中维持仍然很大程度上未知。在这里,我们通过使用缺乏父本等位基因的人类孤雌胚胎干细胞 (hpESC) 来探索印迹调控涉及的机制。我们表明,尽管 hpESC 中的全基因组 DNA 去甲基化会影响大多数印迹 DMR,但许多父本表达基因 (PEG) 仍受到抑制。为了寻找调节 PEG 的因素,我们在单倍体 hpESC 中进行了全基因组 CRISPR/Cas9 筛选。这揭示了 ATF7IP 是一组 PEG 的必需抑制剂,我们进一步表明它也是沉默精子特异性基因所必需的。我们的研究强调了组蛋白修饰在调节印迹基因中的重要作用,并表明亲本印迹和生殖细胞身份之间存在联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/663d/8602306/2459bc863249/41467_2021_26949_Fig1_HTML.jpg

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