• Title of article

    Stepwise Reprogramming of B Cells into Macrophages

  • Author/Authors

    Graf، Thomas نويسنده , , Xie، Huafeng نويسنده , , Ye، Min نويسنده , , Feng، Ru نويسنده ,

  • Issue Information
    هفته نامه با شماره پیاپی سال 2004
  • Pages
    -662
  • From page
    663
  • To page
    0
  • Abstract
    Starting with multipotent progenitors, hematopoietic lineages are specified by lineage-restricted transcription factors. The transcription factors that determine the decision between lymphoid and myeloid cell fates, and the underlying mechanisms, remain largely unknown. Here, we report that enforced expression of C/EBP(alpha) and C/EBP(beta) in differentiated B cells leads to their rapid and efficient reprogramming into macrophages. C/EBPs induce these changes by inhibiting the B cell commitment transcription factor Pax5, leading to the downregulation of its target CD19, and synergizing with endogenous PU.1, an ETS family factor, leading to the upregulation of its target Mac-1 and other myeloid markers. The two processes can be uncoupled, since, in PU.1-deficient pre-B cells, C/EBPs induce CD19 downregulation but not Mac-1 activation. Our observations indicate that C/EBP(alpha) and (beta) remodel the transcription network of B cells into that of macrophages through a series of parallel and sequential changes that require endogenous PU.1.
  • Keywords
    NOx storage/reduction catalysts , NOx release , NO oxidation , Catalyst , Emissions , NOx storage
  • Journal title
    CELL
  • Serial Year
    2004
  • Journal title
    CELL
  • Record number

    102608