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Cell cycle heterogeneity in the small intestinal crypt and maintenance of genome integrity.

机译:细胞周期在小肠隐窝中的异质性和基因组完整性的维持。

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摘要

Stem cell quiescence has been hypothesized to suppress the rate at which genetic mutations accumulate within tissues by reducing the number of divisions a cell undergoes. However, recent studies have suggested that stem cells in the small intestine are rapidly dividing. This observation raises the issue of whether replication related errors are an important contributor to the accumulation of genetic damage and, if so, how genomic integrity is maintained within the small intestine. Here, reporter-marked small intestinal epithelial cells, resulting from mini-chromosome maintenance protein 2 (Mcm2) gene driven Cre-mediated recombination, are shown to be retained at the +1 position within the crypt and to contribute to the intestinal epithelia over long periods. Additionally, we show that the rate of cycling of +1 position Mcm2-expressing stem cells is heterogeneous with cycling times ranging between 1 and 4 days. Further, this heterogeneity depends on the p53 signaling pathway and could provide the basis for retention and expansion, through niche succession and crypt fission, of genetically intact stem cells. This somatic selection process would require active cellular replication.
机译:已经假设干细胞静脉曲张以抑制通过减少细胞经历的划分的数量在组织内积聚的遗传突变的速率。然而,最近的研究表明,小肠中的干细胞正在迅速分裂。该观察结果提出了复制相关错误是否是遗传损伤积累的重要贡献者,如果是的话,基因组完整性如何在小肠内维持。这里,由迷你染色体维持蛋白2(MCM2)基因驱动的CRE介导的重组产生的记者标记的小肠上皮细胞被证明在隐窝内的+1位置保留并为肠上皮延长而导致期间。另外,我们表明,+1位MCM2表达干细胞的循环速率与1至4天之间的循环时间是非均相的。此外,这种异质性取决于P53信号传导途径,并且可以通过基因完整干细胞的利基连续和隐窝裂变来提供保留和膨胀的基础。该躯体选择过程需要有源蜂窝复制。

著录项

  • 来源
    《Stem Cells》 |2010年第7期|共10页
  • 作者

    Pruitt SC; Freeland A; Kudla A;

  • 作者单位

    Department of Molecular and Cellular Biology Roswell Park Cancer Institute Buffalo New York USA.;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医用一般科学;
  • 关键词

  • 入库时间 2022-08-20 05:47:48

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