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Single-molecule imaging of transcription dynamics in somatic stem cells

机译:体细胞干细胞转录动力学的单分子成像

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摘要

Molecular noise is a natural phenomenon that is inherent to all biological systems(1,2). How stochastic processes give rise to the robust outcomes that support tissue homeostasis remains unclear. Here we use single-molecule RNA fluorescent in situ hybridization (smFISH) on mouse stem cells derived from haematopoietic tissue to measure the transcription dynamics of three key genes that encode transcription factors: PU.1 (also known as Spi1), Gata1 and Gata2. We find that infrequent, stochastic bursts of transcription result in the co-expression of these antagonistic transcription factors in the majority of haematopoietic stem and progenitor cells. Moreover, by pairing smFISH with time-lapse microscopy and the analysis of pedigrees, we find that although individual stem-cell clones produce descendants that are in transcriptionally related states-akin to a transcriptional priming phenomenon-the underlying transition dynamics between states are best captured by stochastic and reversible models. As such, a stochastic process can produce cellular behaviours that may be incorrectly inferred to have arisen from deterministic dynamics. We propose a model whereby the intrinsic stochasticity of gene expression facilitates, rather than impedes, the concomitant maintenance of transcriptional plasticity and stem cell robustness. Single-molecule fluorescence in situ hybridization and live-cell imaging are used to study the contribution of transcriptional noise to stem cell heterogeneity, revealing that stochastic transcription dynamics are conducive to concomitant stem-cell maintenance and tissue homeostasis.
机译:分子噪声是所有生物系统固有的天然现象(1,2)。随机过程如何产生支持组织稳态仍然不清楚的强大结果。在这里,我们在源自血液组织衍生的小鼠干细胞上使用单分子RNA荧光荧光(Sm鱼),以测量编码转录因子的三个关键基因的转录动态:PU.1(也称为SPI1),GATA1和GATA2。我们发现罕见,随机转录的转录突发导致这些敌对转录因子在大多数出血茎和祖细胞中的共同表达。此外,通过将Sm鱼与延时显微镜进行配对和分析,我们发现,尽管各个干细胞克隆产生在与转录相关的状态的后代 - 类似于转录引发现象 - 最佳捕获状态之间的潜在转变动态通过随机和可逆模型。这样,随机过程可以产生可能不正确地推断出从确定性动态产生的蜂窝行为。我们提出了一种模型,其中基因表达的内在速度促进,而不是阻碍转录可塑性和干细胞鲁棒性的伴随维持。用于原位杂交和活细胞成像的单分子荧光用于研究转录噪声对干细胞异质性的贡献,揭示随机转录动力学有利于伴随干细胞维持和组织稳态。

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  • 来源
    《Nature》 |2020年第7816期|431-436|共6页
  • 作者单位

    Albert Einstein Coll Med Dept Cell Biol New York NY 10461 USA|Albert Einstein Coll Med Ruth L & David S Gottesman Inst Stem Cell Res & R New York NY 10461 USA;

    Albert Einstein Coll Med Dept Syst & Computat Biol New York NY USA;

    Albert Einstein Coll Med Dept Cell Biol New York NY 10461 USA;

    Albert Einstein Coll Med Dept Cell Biol New York NY 10461 USA;

    Albert Einstein Coll Med Dept Syst & Computat Biol New York NY USA|Albert Einstein Coll Med Dominick P Purpura Dept Neurosci New York NY USA|Albert Einstein Coll Med Dept Pathol New York NY USA|Santa Fe Inst Santa Fe NM 87501 USA;

    Albert Einstein Coll Med Dept Cell Biol New York NY 10461 USA|Albert Einstein Coll Med Dominick P Purpura Dept Neurosci New York NY USA|Albert Einstein Coll Med Dept Anat & Struct Biol New York NY USA|Gruss Lipper Biophoton Ctr Albert Einstein Coll Med New York NY USA|Janelia Res Campus HHMI Ashburn VA USA;

    Albert Einstein Coll Med Dept Cell Biol New York NY 10461 USA|Albert Einstein Coll Med Ruth L & David S Gottesman Inst Stem Cell Res & R New York NY 10461 USA|Montefiore Med Ctr Albert Einstein Coll Med Dept Med Oncol New York NY 10467 USA|Albert Einstein Coll Med Albert Einstein Canc Ctr New York NY 10461 USA;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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