Dev108274 3772..3781

نویسندگان

  • Juan Hou
  • Wei Wei
  • Ranajeet S. Saund
  • Ping Xiang
  • Thomas J. Cunningham
  • Yuyin Yi
  • Olivia Alder
  • Daphne Y. D. Lu
  • Joanne G. A. Savory
  • Nicole A. J. Krentz
  • Rachel Montpetit
  • Rebecca Cullum
  • Nicole Hofs
  • David Lohnes
  • R. Keith Humphries
  • Yojiro Yamanaka
  • Gregg Duester
  • Yukio Saijoh
  • Pamela A. Hoodless
چکیده

Although many regulatory networks involved in defining definitive endoderm have been identified, the mechanisms through which these networks interact to pattern the endoderm are less well understood. To explore the mechanisms involved in midgut patterning, we dissected the transcriptional regulatory elements of nephrocan (Nepn), the earliest known midgut specific gene in mice. We observed that Nepn expression is dramatically reduced inSox17andRaldh2embryos comparedwithwild-type embryos.We further show thatNepn is directly regulated by Sox17 and the retinoic acid (RA) receptor via two enhancer elements located upstream of the gene. Moreover, Nepn expression is modulated by Activin signaling, with high levels inhibiting and low levels enhancing RA-dependent expression. In Foxh1 embryos in which Nodal signaling is reduced, the Nepn expression domain is expanded into the anterior gut region, confirming that Nodal signaling can modulate its expression in vivo. Together, Sox17 is required for Nepn expression in the definitive endoderm, while RA signaling restricts expression to the midgut region. A balance of Nodal/ Activin signaling regulates the anterior boundary of the midgut

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تاریخ انتشار 2014