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Mechanisms of stretch-mediated skin expansion at single-cell resolution

机译:单细胞分辨率下拉伸介导的皮肤膨胀机制

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摘要

The ability of the skin to grow in response to stretching has been exploited in reconstructive surgery(1). Although the response of epidermal cells to stretching has been studied in vitro(2,3), it remains unclear how mechanical forces affect their behaviour in vivo. Here we develop a mouse model in which the consequences of stretching on skin epidermis can be studied at single-cell resolution. Using a multidisciplinary approach that combines clonal analysis with quantitative modelling and single-cell RNA sequencing, we show that stretching induces skin expansion by creating a transient bias in the renewal activity of epidermal stem cells, while a second subpopulation of basal progenitors remains committed to differentiation. Transcriptional and chromatin profiling identifies how cell states and gene-regulatory networks are modulated by stretching. Using pharmacological inhibitors and mouse mutants, we define the step-by-step mechanisms that control stretch-mediated tissue expansion at single-cell resolution in vivo.Single-cell analysis in a mouse model of skin stretching shows that stretching causes a transient expansion bias in a population of epidermal stem cells, which is associated with chromatin remodelling and changes in transcriptional profiles.
机译:在重建手术(1)中,皮肤响应延伸的皮肤增长的能力已经利用。尽管已经在体外研究表皮细胞对拉伸的反应(2,3),但仍然尚不清楚机械力如何影响其体内的行为。在这里,我们开发一种小鼠模型,其中可以在单细胞分辨率下研究皮肤表皮上拉伸的后果。使用多学科方法,将克隆分析与定量建模和单细胞RNA测序相结合,我们表明,通过在表皮干细胞的更新活性中产生瞬态偏压,延伸诱导皮肤膨胀,而基础祖细胞的第二次亚群保持致力于分化。转录和染色质谱鉴定了通过拉伸来调节细胞状态和基因 - 调节网络。使用药理学抑制剂和小鼠突变体,我们定义了控制在体内单细胞分辨率下的拉伸介导的组织膨胀的逐步机制。皮肤拉伸小鼠模型中的单细胞分辨率下的单细胞分辨率表明拉伸导致瞬态膨胀偏差在表皮干细胞的群体中,与染色质重塑和转录谱的变化有关。

著录项

  • 来源
    《Nature》 |2020年第7820期|268-273|共6页
  • 作者单位

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Leuven Dept Human Genet KU Leuven Leuven Belgium|Wellcome Trust Sanger Inst Sanger Inst EBI Single Cell Genom Ctr Hinxton England;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Leuven Dept Human Genet KU Leuven Leuven Belgium|Wellcome Trust Sanger Inst Sanger Inst EBI Single Cell Genom Ctr Hinxton England;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium;

    Electron Microscopy Platform VIB Bio Imaging Core Leuven Belgium;

    Electron Microscopy Platform VIB Bio Imaging Core Leuven Belgium;

    Univ Cambridge Wellcome Trust Canc Res UK Gurdon Inst Cambridge England|Univ Cambridge Stem Cell Inst MRC Wellcome Trust Cambridge England;

    Catholic Univ Louvain Inst Neurosci Dev Neurobiol Brussels Belgium;

    Univ Leuven Dept Human Genet KU Leuven Leuven Belgium|Wellcome Trust Sanger Inst Sanger Inst EBI Single Cell Genom Ctr Hinxton England;

    Univ Cambridge Wellcome Trust Canc Res UK Gurdon Inst Cambridge England|Univ Cambridge Stem Cell Inst MRC Wellcome Trust Cambridge England|Univ Cambridge Ctr Math Sci Dept Appl Math & Theoret Phys Cambridge England;

    Univ Libre Bruxelles Lab Stem Cells & Canc Brussels Belgium|Univ Libre Bruxelles WELBIO Brussels Belgium;

  • 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);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-18 22:15:27

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