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首页> 外文期刊>Cell stem cell >The BAF and PRC2 Complex Subunits Dpf2 and Eed Antagonistically Converge on Tbx3 to Control ESC Differentiation
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The BAF and PRC2 Complex Subunits Dpf2 and Eed Antagonistically Converge on Tbx3 to Control ESC Differentiation

机译:BAF和PRC2复杂亚基DPF2和EED对抗TBX3对抗控制ESC差异化

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摘要

BAF complexes are composed of different subunits with varying functional and developmental roles, although many subunits have not been examined in depth. Here we show that the Baf45 subunit Dpf2 maintains pluripotency and ESC differentiation potential. Dpf2 co-occupies enhancers with Oct4, Sox2, p300, and the BAF subunit Brg1, and deleting Dpf2 perturbs ESC self-renewal, induces repression of Tbx3, and impairs mesendodermal differentiation withoutdramatically altering Brg1 localization. Mesendodermal differentiation can be rescued by restoring Tbx3 expression, whose distal enhancer is positively regulated by Dpf2-dependent H3K27ac maintenance and recruitment of pluripotency TFs and Brg1. In contrast, the PRC2 subunit Eed binds an intragenic Tbx3 enhancer to oppose Dpf2-dependent Tbx3 expression and mesendodermal differentiation. The PRC2 subunit Ezh2 likewise opposes Dpf2-dependent differentiation through a distinct mechanism involving Nanog repression. Together, these findings delineate distinct mechanistic roles for specific BAF and PRC2 subunits during ESC differentiation.
机译:BAF复合物由不同的亚基组成,具有不同的功能和发育角色,尽管未经深入检查许多亚基。在这里,我们表明BAF45亚基DPF2维持多能性和ESC分化潜力。 DPF2与OCT4,SOX2,P300和BAF亚单位BRG1共同占用增强剂,并删除DPF2 Perturbs ESC自我更新,诱导TBX3的抑制,并损害结论映射分化,无模糊地改变BRG1定位。通过恢复Tbx3表达可以救出中胚层分化,其远端增强剂通过DPF2依赖性H3K27AC阳性调节,多能TFS和BRG1募集。相反,PRC2亚基ED结合腺瘤TBX3增强子以阻抗DPF2依赖性TBX3表达和中畸形分化。通过涉及纳米记抑制的不同机制,PRC2亚基EzH2同样反对DPF2依赖性分化。这些发现在ESC分化期间描绘了特定BAF和PRC2亚基的不同机械角色。

著录项

  • 来源
    《Cell stem cell》 |2019年第1期|共15页
  • 作者单位

    Soochow Univ Cam Su Genom Resource Ctr Suzhou 215123 Peoples R China;

    Univ Calif Los Angeles David Geffen Sch Med Dept Biol &

    Chem Los Angeles CA 90095 USA;

    Wellcome Sanger Inst Hinxton CB10 1SA England;

    Soochow Univ Cam Su Genom Resource Ctr Suzhou 215123 Peoples R China;

    KTH Royal Inst Technol Div Gene Technol Sci Life Lab S-10691 Stockholm Sweden;

    Chester Beatty Labs Inst Canc Res London England;

    Soochow Univ Cam Su Genom Resource Ctr Suzhou 215123 Peoples R China;

    Max Planck Inst Mol Biomed Dept Cell &

    Dev Biol Rontgenstr 20 D-48149 Munster Germany;

    Wellcome Sanger Inst Hinxton CB10 1SA England;

    Wellcome Sanger Inst Hinxton CB10 1SA England;

    Chester Beatty Labs Inst Canc Res London England;

    Chester Beatty Labs Inst Canc Res London England;

    Univ Cambridge Wellcome Trust Med Res Council Stem Cell Inst Tennis Court Rd Cambridge CB2 1QR;

    Univ Calif San Diego Dept Pathol La Jolla CA 92093 USA;

    Max Planck Inst Mol Biomed Dept Cell &

    Dev Biol Rontgenstr 20 D-48149 Munster Germany;

    KTH Royal Inst Technol Div Gene Technol Sci Life Lab S-10691 Stockholm Sweden;

    Univ Calif Los Angeles David Geffen Sch Med Dept Biol &

    Chem Los Angeles CA 90095 USA;

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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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