FETAL PANCREAS ALLOGRAFTS FOR REVERSAL OF DIABETES IN RATS
- 1 January 1982
- journal article
- research article
- Published by Wolters Kluwer Health in Transplantation
- Vol. 33 (1) , 3-11
- https://doi.org/10.1097/00007890-198201000-00002
Abstract
Specific unresponsiveness to LEW [Lewis rat] whole fetal pancreases was induced in F344 rats across non-RT1 incompatibilities. The treatment regimen was a modification of that developed by others and used an i.v. injection of donor liver extracts (equivalent to 250-500 mg wet tissues) between days -18 and -24 followed by a single i.p. injection each of procarbazine hydrochloride (1/3 of the LD50 dose) and 0.5 ml of antilymphocyte serum (ALS) within a few days of transplantation. Complete and life-term (> 1 yr) reversal of streptozotocin (SZ)-induced diabetes was observed in 13 of 16 treated recipients, while the reversal of diabetes was only transient in 2 recipients as a result of graft rejection which occurred between days 30 and 50. The remaining 1 recipient did not respond to the treatment. Allograft viability was confirmed by the visual observation and histological examination of tissues, by the recurrence of diabetes after the graft removal, and by the reversal of diabetes in the secondary recipients in which long-term surviving allografts were retransplanted. Specificity of the induced unresponsiveness was demonstrated by the prolonged survival times of donor-type skin but the normal rejection of 3rd-party skin which was grafted onto the diabetes-reversed F344 recipients carrying viable LEW pancreases. Prolonged but limited survival times of donor-type skin grafts suggested that the induced unresponsiveness is specific to donor alloantigens and organ-specific antigens. This immunosuppressed state was transferable into ALS-treated syngeneic F344 rats by nylon-wool-nonadherent spleen cells. Thus, LEW skin grafts survived for 30 days in ALS-treated F344 rats receiving test spleen cells, while those in controls survived for 19 days. LEW pancreases surviving for more than 300 days were fully capable of eliciting rejection reaction when the grafts were retransplanted into a nonimmunosuppressed secondary F344 recipient along with the primary host kidney.This publication has 7 references indexed in Scilit:
- FETAL PANCREAS ALLOGRAFTS FOR REVERSAL OF DIABETES IN RATSTransplantation, 1980
- Prolongation of Islet Allograft Survival Following in Vitro Culture (24°C) and a Single Injection of ALSScience, 1979
- SPECIFIC UNRESPONSIVENESS TO SKIN ALLOGRAFTS IN MICE V. SYNERGY BETWEEN DONOR TISSUE EXTRACT, PROCARBAZINE HYDROCHLORIDE, AND ANTILYMPHOCYTE SERUM IN CREATING A LONG-LASTING UNRESPONSIVENESS MEDIATED BY SUPPRESSOR T CELLSTransplantation, 1979
- REVERSAL OF DIABETES IN RATS USING FETAL PANCREASES STORED AT −196 ,CTransplantation, 1978
- Induction of specific tissue transplantation tolerance using fractionated total lymphoid irradiation in adult mice: long-term survival of allogeneic bone marrow and skin grafts.The Journal of Experimental Medicine, 1977
- Coated Charcoal Immunoassay of InsulinJournal of Clinical Endocrinology & Metabolism, 1965
- Observations with differential stains on human islets of Langerhans1941