Zfx Controls the Self-Renewal of Embryonic and Hematopoietic Stem Cells

نویسندگان

  • Jose M. Galan-Caridad
  • Sivan Harel
  • Teresita L. Arenzana
  • Z. Esther Hou
  • Fiona K. Doetsch
  • Leonid A. Mirny
  • Boris Reizis
چکیده

Stem cells (SC) exhibit a unique capacity for self-renewal in an undifferentiated state. It is unclear whether the self-renewal of pluripotent embryonic SC (ESC) and of tissue-specific adult SC such as hematopoietic SC (HSC) is controlled by common mechanisms. The deletion of transcription factor Zfx impaired the self-renewal but not the differentiation capacity of murine ESC; conversely, Zfx overexpression facilitated ESC self-renewal by opposing differentiation. Furthermore, Zfx deletion abolished the maintenance of adult HSC but did not affect erythromyeloid progenitors or fetal HSC. Zfx-deficient ESC and HSC showed increased apoptosis and SC-specific upregulation of stress-inducible genes. Zfx directly activated common target genes in ESC and HSC, as well as ESC-specific target genes including ESC self-renewal regulators Tbx3 and Tcl1. These studies identify Zfx as a shared transcriptional regulator of ESC and HSC, suggesting a common genetic basis of self-renewal in embryonic and adult SC.

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عنوان ژورنال:
  • Cell

دوره 129  شماره 

صفحات  -

تاریخ انتشار 2007