| Pancreatic and duodenal homeobox 1 (Pdx1) was one of the first pancreas specific genes isolated. It is expressed in early pancreatic buds, throughout the duodenum and localized to insulin producing cells in the adult. Pdx1 plays a fundamental role in pancreas development as the loss-of-function of Pdx1 in mice and frogs result in absence of pancreatic tissue. In humans, Pdx1 homozygous mutations lead to pancreas agenesis, while heterozygous mutations result in type 2 diabetes. Our laboratory studies the role of Pdx1 in promoting ectopic pancreatic cell fates. Using Xenopus laevis as a model, we previously showed that the overexpression of a modified form of Pdx1, Pdx1-VP16, is sufficient to convert liver to pancreas. Whether Pdx1 is able to promote ectopic pancreas in naive endoderm has yet to be determined. To achieve this, Pdx1 mRNA was overexpressed in the anterior endoderm. The overexpression resulted in ectopic tissue with reduced expression of exocrine and endocrine differentiation markers. In addition, stomach, duodenum and liver organogenesis was severely perturbed. To ascertain the identity of this ectopic tissue, microarray analysis was performed which confirmed the reduction in pancreatic endocrine and exocrine cells as well as the reduction in stomach, duodenum and hepatic tissue. Moreover, the genes highly upregulated suggest a pancreatic stellate cell phenotype. The information obtained from the gain-of-function analysis will help explain the role of this transcription factor in regulating the initial stages of pancreatic cell fate specification. |
