Islet mass and β-cell proliferation is decreased in Hhip–/– embryos (Hip1 in figure). Islet mass and β-cell proliferation is decreased in Hhip–/– embryos.

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Islet mass and β-cell proliferation is decreased in Hhip–/– embryos (Hip1 in figure). Islet mass and β-cell proliferation is decreased in Hhip–/– embryos (Hip1 in figure). Islets were stained with antibodies directed against centrally located insulin (green) and marginally located glucagon producing cells (red). Hhip function is required for normal islet morphogenesis (A,B). Clusters of insulin- and glucagon-positive cells form but are significantly smaller than the ones in control embryos (wild-type or heterozygotes, compare B with A). To adjust for differences in body mass, pancreas weight and islet area were divided by body weight. (C, blue, control, n=6; red, Hhip–/–, n=5; *P<0.05, **P<0.01). Quantification of islet areas revealed a 45% reduction that is more pronounced than the general loss of pancreatic tissue (C, blue, control; red, Hhip–/–). The reduction in islet mass is due to the loss of larger islets (>4000 μm2) while the number of smaller islets (>4000 μm2) is maintained in Hhip mutants (D, blue, control, n=5; red, Hhip–/–, n=5; #no significant difference, **P<0.01). Staining for the nuclear marker Ki-67 showed that proliferation of β-cells at E18.5 is reduced by 39% (E, blue, control, n=3; red, Hhip–/–, n=5; *P<0.05). Changes in islet morphogenesis andβ -cell proliferation are not due to incomplete cell differentiation (F-I). β-cells express mature markers, including Pdx1 (F,G; insulin, green; Pdx1, red) and glucose transporter 2 (H,I; insulin, green; Glut2, red). Error bars shown are ±s.d. Hiroshi Kawahira et al. Development 2003;130:4871-4879 © 2003.