Figure 4. Autoimmunity is ameliorated by high levels of endogenous islet cells' VTCN1.

(A) Representative immunofluorescent images (left) and quantitative analysis (right) of pancreatic islets from B6^g7 mice 20 days after reception of 10⁷ splenocytes from acutely diabetic NOD mouse (Adoptive transfer) or vehicle solution (vehicle) (n=3-5 mice/group). Overlay of VTCN1 (red), insulin (green), and DNA (blue) is shown in the third column. (B) Representative images of pancreatic cryosections from NOD-scid mice of indicated ages stained for VTCN1 (red) and insulin (green). (C) Changes in the VTCN1 immunoreactivity in islets from vehicle-transferred (Sham) or splenocytes-transferred (Transferred) NOD-scid and irradiated B6^g7 mice 3 weeks after adoptive transfers of 10⁷ splenocytes from acutely diabetic NOD mice (n=3-4 mice/group). (D) Representative images (left) and quantitative analysis (right) of EdU-positive T cells within insulitic lesions of adoptively transferred, as in C, NOD-scid and B6^g7-Rag1^-/-mice, 3 weeks after transfer (n=3-4 mice/group). Scale bars, 50 μm; **p<0.01, ***p<0.001.