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首页> 外文期刊>Cell stem cell >SUMO Safeguards Somatic and Pluripotent Cell Identities by Enforcing Distinct Chromatin States
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SUMO Safeguards Somatic and Pluripotent Cell Identities by Enforcing Distinct Chromatin States

机译:通过实施不同的染色质态,SUMO保障体细胞和多能细胞标识

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摘要

Understanding general principles that safeguard cellular identity should reveal critical insights into common mechanisms underlying specification of varied cell types. Here, we show that SUMO modification acts to stabilize cell fate in a variety of contexts. Hyposumoylation enhances pluripotency reprogramming in vitro and in vivo, increases lineage transdifferentiation, and facilitates leukemic cell differentiation. Suppressing sumoylation in embryonic stem cells (ESCs) promotes their conversion into 2-cell-embryo-like (2C-like) cells. During reprogramming to pluripotency, SUMO functions on fibroblastic enhancers to retain somatic transcription factors together with Oct4, Sox2, and Klf4, thus impeding somatic enhancer inactivation. In contrast, in ESCs, SUMO functions on heterochromatin to silence the 2C program, maintaining both proper H3K9me3 levels genome-wide and repression of the Dux locus by triggering recruitment of the sumoylated PRC1.6 and Kap/Setdb1 repressive complexes. Together, these studies show that SUMO acts on chromatin as a glue to stabilize key determinants of somatic and pluripotent states.
机译:了解保护蜂窝身份的一般原则应该揭示对不同细胞类型规范的普遍机制的关键见解。在这里,我们表明Sumo修改起到稳定细胞命运的各种背景。脱溶胶增强多能性重编程在体外和体内,增加谱系转移,并促进白血病细胞分化。抑制胚胎干细胞(ESC)中的平均促进其转化为2细胞 - 胚状(2C样)细胞。在对多能性的重新编程期间,SUMO功能在成纤维细胞增强子上,以将体细胞转录因子与OCT4,SOX2和KLF4一起保留,从而阻碍体细胞增强剂失活。相比之下,在ESC中,SUMO在异铬胺偶联以沉默2C程序,通过触发友好的PRC1.6和KAP / SETDB1压制复合物的募集来维持Dux Locus的适当H3K9ME3水平和抑制Dux Locus。这些研究在一起表明,Sumo作用于染色质作为胶水,以稳定体细胞和多能态的关键决定因素。

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  • 来源
    《Cell stem cell》 |2018年第5期|共24页
  • 作者单位

    Inst Pasteur Nucl Org &

    Oncogenesis Unit Equipe Labellisee Ligue Natl Canc F-75015 Paris France;

    Inst Pasteur Nucl Org &

    Oncogenesis Unit Equipe Labellisee Ligue Natl Canc F-75015 Paris France;

    Inst Pasteur Bioinformat &

    Biostat Hub C3BI USR 3756 F-75015 Paris France;

    Inst Pasteur Cellular Plastic &

    Dis Modelling Unit F-75015 Paris France;

    Helmholtz Zentrum Munchen Inst Epigenet &

    Stem Cells Munich Germany;

    Inst Pasteur Nucl Org &

    Oncogenesis Unit Equipe Labellisee Ligue Natl Canc F-75015 Paris France;

    Helmholtz Zentrum Munchen Inst Epigenet &

    Stem Cells Munich Germany;

    Inst Pasteur Expt Neuropathol Unit F-75015 Paris France;

    Inst Pasteur Cellular Plastic &

    Dis Modelling Unit F-75015 Paris France;

    Univ Montpellier CNRS Inst Genet Mol Montpellier Montpellier France;

    Inst Pasteur Nucl Org &

    Oncogenesis Unit Equipe Labellisee Ligue Natl Canc F-75015 Paris France;

    Helmholtz Zentrum Munchen Inst Epigenet &

    Stem Cells Munich Germany;

    Inst Pasteur Nucl Org &

    Oncogenesis Unit Equipe Labellisee Ligue Natl Canc F-75015 Paris France;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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