• Title of article

    Developmental Fate and Cellular Maturity Encoded in Human Regulatory DNA Landscapes

  • Author/Authors

    Andrew B. Stergachis، نويسنده , , Shane Neph، نويسنده , , Alex Reynolds، نويسنده , , Richard Humbert، نويسنده , , Brady Miller، نويسنده , , Sharon L. Paige، نويسنده , , Benjamin Vernot، نويسنده , , Jeffrey B. Cheng، نويسنده , , Robert E. Thurman، نويسنده , , Richard Sandstrom، نويسنده , , Eric Haugen، نويسنده , , Shelly Heimfeld، نويسنده , , Charles E. Murry، نويسنده , , Joshua M. Akey، نويسنده , , John A. Stamatoyannopoulos، نويسنده ,

  • Issue Information
    هفته نامه با شماره پیاپی سال 2013
  • Pages
    16
  • From page
    888
  • To page
    903
  • Abstract
    Cellular-state information between generations of developing cells may be propagated via regulatory regions. We report consistent patterns of gain and loss of DNase I-hypersensitive sites (DHSs) as cells progress from embryonic stem cells (ESCs) to terminal fates. DHS patterns alone convey rich information about cell fate and lineage relationships distinct from information conveyed by gene expression. Developing cells share a proportion of their DHS landscapes with ESCs; that proportion decreases continuously in each cell type as differentiation progresses, providing a quantitative benchmark of developmental maturity. Developmentally stable DHSs densely encode binding sites for transcription factors involved in autoregulatory feedback circuits. In contrast to normal cells, cancer cells extensively reactivate silenced ESC DHSs and those from developmental programs external to the cell lineage from which the malignancy derives. Our results point to changes in regulatory DNA landscapes as quantitative indicators of cell-fate transitions, lineage relationships, and dysfunction.
  • Journal title
    CELL
  • Serial Year
    2013
  • Journal title
    CELL
  • Record number

    1021859