Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
3318086 | Pancreatology | 2010 | 11 Pages |
Abstract
Background/Aims: Midgut formation in Drosophilamelanogasteris dependent upon the integrity of a signaling loop in the endoderm which requires the TGFβ-related peptide, Decapentaplegic, and the Hoxtranscription factor, Labial. Interestingly, although Labial-like homeobox genes are present in mammals, their participation in endoderm morphogenesis is not clearly understood. Methods: We report the cloning, expression, localization, TGFβ inducibility, and biochemical properties of the mammalian Labial-like homeobox, HoxA1, in exocrine pancreatic cells that are embryologically derived from the gut endoderm. Results: HoxA1 is expressed in pancreatic cell populations as two alternatively spliced messages, encoding proteins that share their N-terminal domain, but either lack or include the homeobox at the C-terminus. Transcriptional regulatory assays demonstratethat the shared N-terminal domain behaves as a strong transcriptional activator in exocrine pancreatic cells. HoxA1 is an early response gene for TGFβ1 in pancreatic epithelial cell populations and HoxA1 protein co-localizes with TGFβ1 receptors in the embryonic pancreatic epithelium at a time when exocrine pancreatic morphogenesis occurs (days E16 and E17). Conclusions: These results report a role for HoxA1 in linking TGFβ-mediated signaling to gene expression in pancreatic epithelial cell populations, thus suggesting a high degree of conservation for a TGFβ/labial signaling loop in endoderm-derived cells between Drosophila and mammals.
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Authors
Gwen A. Lomberk, Issei Imoto, Brian Gebelein, Raul Urrutia, Tiffany A. Cook,