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Autoimmune destruction of islets transplanted into RT6-depleted diabetes-resistant BB/Wor rats.

  1. P A Gottlieb,
  2. J P Berrios,
  3. G Mariani,
  4. E S Handler,
  5. D Greiner,
  6. J P Mordes and
  7. A A Rossini
  1. Department of Medicine, University of Massachusetts Medical School, Worcester 01655.

    Abstract

    We report a novel animal model of islet transplantation that distinguishes recurrence of autoimmunity from allograft rejection. In this study, diabetes-resistant (DR) BB rats, less than 1% of which develop spontaneous diabetes, were made hyperglycemic by either a single injection of streptozocin (STZ) or in vivo immune elimination of a regulatory T-lymphocyte subset that expresses the RT6 alloantigen. DR islet grafts were then transplanted into both groups. DR transplants into STZ-induced diabetic DR rats produced long-term normoglycemia. In contrast, DR transplants into DR rats that had been treated with anti-RT6 monoclonal antibody were all destroyed within an average of 4 days. Allogeneic islets transplanted into both STZ-induced and RT6-depleted diabetic DR rats were rejected within a mean of 3 days. We conclude that failure of DR islet grafts in RT6-depleted diabetic DR BB rats represents recurrent autoimmunity.

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