The diabetes gene Pdx1 regulates the transcriptional network of pancreatic endocrine progenitor cells in mice
Jennifer M. Oliver-Krasinski, … , Klaus H. Kaestner, Doris A. Stoffers
Jennifer M. Oliver-Krasinski, … , Klaus H. Kaestner, Doris A. Stoffers
Published June 1, 2009
Citation Information: J Clin Invest. 2009;119(7):1888-1898. https://doi.org/10.1172/JCI37028.
View: Text | PDF
Research Article Metabolism

The diabetes gene Pdx1 regulates the transcriptional network of pancreatic endocrine progenitor cells in mice

Abstract

Heterozygous mutations in the gene encoding the pancreatic homeodomain transcription factor pancreatic duodenal homeobox 1 (PDX1) are associated with maturity onset diabetes of the young, type 4 (MODY4) and type 2 diabetes. Pdx1 governs the early embryonic development of the pancreas and the later differentiation of the insulin-producing islet β cells of the endocrine compartment. We derived a Pdx1 hypomorphic allele that reveals a role for Pdx1 in the specification of endocrine progenitors. Mice homozygous for this allele displayed a selective reduction in endocrine lineages associated with decreased numbers of endocrine progenitors and a marked reduction in levels of mRNA encoding the proendocrine transcription factor neurogenin 3 (Ngn3). During development, Pdx1 occupies an evolutionarily conserved enhancer region of Ngn3 and interacts with the transcription factor one cut homeobox 1 (Hnf6) to activate this enhancer. Furthermore, mRNA levels of all 4 members of the transcription factor network that regulates Ngn3 expression, SRY-box containing gene 9 (Sox9), Hnf6, Hnf1b, and forkhead box A2 (Foxa2), were decreased in homozygous mice. Pdx1 also occupied regulatory sequences in Foxa2 and Hnf1b. Thus, Pdx1 contributes to specification of endocrine progenitors both by regulating expression of Ngn3 directly and by participating in a cross-regulatory transcription factor network during early pancreas development. These results provide insights that may be applicable to β cell replacement strategies involving the guided differentiation of ES cells or other progenitor cell types into the β cell lineage, and they suggest a molecular mechanism whereby human PDX1 mutations cause diabetes.

Authors

Jennifer M. Oliver-Krasinski, Margaret T. Kasner, Juxiang Yang, Michael F. Crutchlow, Anil K. Rustgi, Klaus H. Kaestner, Doris A. Stoffers

×

Figure 2

Dose-dependent regulation of pancreas organogenesis.

Options: View larger image (or click on image) Download as PowerPoint
Dose-dependent regulation of pancreas organogenesis. (A–E) Normal pancre...
(AE) Normal pancreas organogenesis in Pdx1ΔC/ΔC mice. (A) Foregut and accessory organs were dissected from newborn animals. The pancreas is highlighted by a black dotted line. (B) Body weights and (C) pancreatic weights were also measured at P1 (n = 6–15 per group). (D and E) Development of overt diabetes in Pdx1ΔC/ΔC mice. (D) Random blood glucose levels were measured at birth and (E) followed for 3 weeks in Pdx1ΔC/ΔC (triangles), Pdx1+/ΔC (squares), and Pdx1+/+ (circles) littermates (n = 6–21 per group; *P < 0.003 compared with both other groups). (FI) Pancreatic hypoplasia in Pdx1ΔC/– mice. (F) Foregut and accessory organs were dissected from newborn animals. The pancreata from wild-type (left panel) and Pdx1ΔC/– (right panel) mice are highlighted by the black dotted line. (G) Body weights, (H) pancreatic weights, and (I) random blood glucose levels were measured in wild-type and Pdx1ΔC/– littermates at P1 (n = 5 per group; *P < 0.003).