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FK-506 AND METHOTREXATE PREVENT GRAFT-VERSUS-HOST DISEASE IN DOGS GIVEN 9.2 GY TOTAL-BODY IRRADIATION AND MARROW GRAFTS FROM UNRELATED DOG LEUKOCYTE ANTIGEN-NONIDENTICAL DONORS

Authors

STORB R RAFF RF APPELBAUM FR DEEG HJ FITZSIMMONS W GRAHAM TC PEPE M PETTINGER M SALE G VANDERJAGT R SCHUENING FG

Citation

R. Storb et al., FK-506 AND METHOTREXATE PREVENT GRAFT-VERSUS-HOST DISEASE IN DOGS GIVEN 9.2 GY TOTAL-BODY IRRADIATION AND MARROW GRAFTS FROM UNRELATED DOG LEUKOCYTE ANTIGEN-NONIDENTICAL DONORS, Transplantation, 56(4), 1993, pp. 800-807

Citations number

Categorie Soggetti

Immunology,Surgery

Journal title

Transplantation → ACNP

ISSN journal

00411337

Volume

Issue

Year of publication

1993

Pages

800 - 807

Database

ISI

SICI code

0041-1337(1993)56:4<800:FAMPGD>2.0.ZU;2-J

Abstract

FK-506 was evaluated either alone or combined with methotrexate (MTX) for prevention of graft-versus-host disease (GVHD) in dogs given 9.2 G y total body irradiation and dog leukocyte antigen-nonidentical unrela ted marrow grafts. Studies with marrow autografts showed gut toxicity and weight loss to be major side effects of FK-506. There was no hemat opoietic toxicity with FK-506. In an initial allograft study, 5 dogs w ere given FK-506 intramuscularly at 0.3 mg/kg/day from days 0 to 8 and then orally at 0.5 mg/kg/day. All 5 died, 3 with intussusception most likely due to FK-506 toxicity, 1 with graft failure, and 1 with GVHD. Subsequently, the FK-506 dose was reduced and these drug schedules we re used: FK-506 days 0-8 at 0.15 mg/kg/day i.m. and then orally at 0.5 mg/kg/day until day 90, with or without MTX intravenously at 0.4 mg/k g days 1, 3, 6, and 11. Twenty allografts were done, 10 with FK-506 al one, and 10 with MTX/FK-506. Results were compared with those in concu rrent and historical controls given either no immunosuppression (n=64) , MTX (n=114), CsA (n=15), or MTX/CsA (n=17). Five of 20 current dogs died with intussusception, too early to be evaluated for GVHD. The 10 dogs given FK-506 alone survived significantly better than those not g iven immunosuppression but not differently from those given short-term MTX or CsA alone. Three died from toxicity, 2 with graft failure, and 4 with GVHD. Only 1 dog became a long-term survivor, and this dog ina dvertently received a single dose of MTX on day 7. Two of 10 dogs give n MTX/FK-506 died from toxicity, 1 died with graft failure, 2 died wit h GVHD, and 5 became long-term survivors, a result that is significant ly better than seen with either drug alone and similar to that seen wi th MTX/CsA. Four of the 5 survivors had no clinical GVHD. FK-506 blood levels were 15-35 ng/ml between days 8 and 15, when gut toxicity was most severe. Thereafter, levels were approximately 5 ng/ml. In conclus ion, FK-506 prolonged survival of recipients of dog leukocyte antigen- nonidentical unrelated marrow grafts. When FK-506 was combined with MT X, graft-host tolerance was induced in 50% of dogs, even though FK-506 was stopped on day 90.