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Non-coding Transcription Instructs Chromatin Folding and Compartmentalization to Dictate Enhancer-Promoter Communication and T Cell Fate

机译:非编码转录指示染色质折叠和分区化以决定增强剂 - 启动子通信和T细胞命运

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摘要

It is now established that Bcl11b specifies T cell fate. Here, we show that in developing T cells, the Bcl11b enhancer repositioned from the lamina to the nuclear interior. Our search for factors that relocalized the Bcl11b enhancer identified a non-coding RNA named ThymoD (thymocyte differentiation factor). ThymoD-deficient mice displayed a block at the onset of T cell development and developed lymphoid malignancies. We found that ThymoD transcription promoted demethylation at CTCF bound sites and activated cohesin-dependent looping to reposition the Bcl11b enhancer from the lamina to the nuclear interior and to juxtapose the Bcl11b enhancer and promoter into a single-loop domain. These large-scale changes in nuclear architecture were associated with the deposition of activating epigenetic marks across the loop domain, plausibly facilitating phase separation. These data indicate how, during developmental progression and tumor suppression, noncoding transcription orchestrates chromatin folding and compartmentalization to direct with high precision enhancer-promoter communication.
机译:现在建立了BCL11B指定T细胞命运。在这里,我们表明,在开发T细胞中,BCL11B增强剂从椎板重新定位到核内部。我们寻找重新定位BCL11B增强子的因素鉴定了名为Thymod(胸腺细胞分化因子)的非编码RNA。胸腺缺陷小鼠在T细胞发育的发作和发育淋巴恶恶性肿瘤时显示出块。我们发现胸腺转录在CTCF结合位点促进去甲基化,并激活依赖辛酸依赖性循环,以将BCL11B增强子从椎板重新定位到核内部,并将BCL11B增强子和启动子并置成单环结构域。这些大规模的核结构变化与在环形结构域中激活外膜遗传标记的沉积相关,可编征促进相分离。这些数据表明,在发育进展和肿瘤抑制期间,非编码转录核对染色质折叠和分区化,以指导高精度增强剂 - 启动子通信。

著录项

  • 来源
    《Cell》 |2017年第1期|共35页
  • 作者单位

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Med Ctr Computat Biol &

    Bioinformat Inst Genom Med La Jolla CA 92093 USA;

    Univ Calif San Diego Dept Med Ctr Computat Biol &

    Bioinformat Inst Genom Med La Jolla CA 92093 USA;

    Fox Chase Canc Ctr Blood Cell Dev &

    Funct 333 Cottman Ave Philadelphia PA 19111 USA;

    Fox Chase Canc Ctr Blood Cell Dev &

    Funct 333 Cottman Ave Philadelphia PA 19111 USA;

    Univ Calif San Diego Dept Mol Biol La Jolla CA 92093 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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