AUTOIMMUNE DIABETES AS A CONSEQUENCE OF LOCALLY PRODUCED INTERLEUKIN-2

Heath, WR; Allison, J; Hoffmann, MW; SCHONRICH, G; Hammerling, G; Arnold, B; Miller, JFAP

Author(s): Heath, WR; Allison, J; Hoffmann, MW; SCHONRICH, G; Hammerling, G; Arnold, B; Miller, JFAP;
Details: Publication Year 1992-10-08,Volume 359,Issue #6395,Page 547-549
Journal Title: NATURE
Publication Type: Journal Article
Abstract: DURING cell differentiation in the thymus, self-reactive T cells can be generated. The majority of these seem to be deleted after intrathymic encounter with the relevant autoantigen1. As all self antigens are unlikely to be present in the thymus, some autoreactive T cells may escape censorship. Here we study the fate of these cells using transgenic mice expressing the class I molecule H-2K(b) (K(b)) in the insulin-producing beta-cells of the pancreas2,3. These mice were crossed with mice transgenic for genes encoding a K(b)-specific T-cell antigen receptor (TCR)4 which could be detected using a clonotype-specific monoclonal antibody5. Although T cells expressing the highest level of transgenic TCR were deleted intrathymically in double-transgenic mice, K(b)-specific T cells were detected in the periphery. These cells caused the rejection of K(b)-expressing skin grafts, but ignored islet K(b) antigens even after priming. But when double-transgenic mice were crossed with transgenic mice expressing the lymphokine interleukin-2 in the pancreatic beta-cells6, there was a rapid onset of diabetes. These results indicate that autoreactive T cells that ignore self antigens may cause autoimmune diabetes when provided with exogenous 'help' in the form of interleukin-2.
Publisher: MACMILLAN MAGAZINES LTD
Keywords: RECEPTOR TRANSGENIC MICE; VIRUS-INFECTION; T-CELLS; TOLERANCE; MOLECULES; MECHANISM; INDUCTION
Publisher's Version: https://doi.org/10.1038/359547a0
Terms of Use/Rights Notice: Refer to copyright notice on published article.

Creation Date: 1992-10-08 12:00:00