Foxl1-Cre-marked adult hepatic progenitors have clonogenic and bilineage differentiation potential.

نویسندگان

  • Soona Shin
  • Gabriel Walton
  • Reina Aoki
  • Karrie Brondell
  • Jonathan Schug
  • Alan Fox
  • Olga Smirnova
  • Craig Dorrell
  • Laura Erker
  • Andrew S Chu
  • Rebecca G Wells
  • Markus Grompe
  • Linda E Greenbaum
  • Klaus H Kaestner
چکیده

Isolation of hepatic progenitor cells is a promising approach for cell replacement therapy of chronic liver disease. The winged helix transcription factor Foxl1 is a marker for progenitor cells and their descendants in the mouse liver in vivo. Here, we purify progenitor cells from Foxl1-Cre; RosaYFP mice and evaluate their proliferative and differentiation potential in vitro. Treatment of Foxl1-Cre; RosaYFP mice with a 3,5-diethoxycarbonyl-1,4-dihydrocollidine diet led to an increase of the percentage of YFP-labeled Foxl1(+) cells. Clonogenic assays demonstrated that up to 3.6% of Foxl1(+) cells had proliferative potential. Foxl1(+) cells differentiated into cholangiocytes and hepatocytes in vitro, depending on the culture condition employed. Microarray analyses indicated that Foxl1(+) cells express stem cell markers such as Prom1 as well as differentiation markers such as Ck19 and Hnf4a. Thus, the Foxl1-Cre; RosaYFP model allows for easy isolation of adult hepatic progenitor cells that can be expanded and differentiated in culture.

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عنوان ژورنال:
  • Genes & development

دوره 25 11  شماره 

صفحات  -

تاریخ انتشار 2011