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Surgery ; 110(1): 87-98, 1991 Jul.
Article de Anglais | MEDLINE | ID: mdl-1714104

RÉSUMÉ

Abdominal multivisceral allotransplantation (MVTX) from Brown Norway donor rats to Lewis recipient rats was performed under a 14-day course of low (0.32 mg/kg) or high-dose (0.64 mg/kg) intramuscular FK 506 to which weekly further injections were added in some of the high-dose animals. With all three regimens, long survival was frequently achieved with good intestinal adsorption and weight gain, but histopathologic evidence of intestinal rejection existed in the most lightly treated animals. The liver, stomach, and pancreas had only minor abnormalities. Rejection of isolated intestinal grafts was more difficult to control based on histopathologic criteria, and satisfactory results were obtained only with the most aggressive treatment protocol, suggesting that the liver in the MVTX had provided an advantage to the companion organs of the graft, of which the intestine was most vulnerable. Histopathologically, the lymphoid elements of the intestine, including the Peyer's patches, appeared to be the most immunogenic component of the intestine. Epithelium near lymphoid areas was secondarily involved with villous atrophy, cryptitis, and abscess formation. Beginning within 12 days in successful MVTX experiments, the lymphoreticular components of the graft intestine, including the Peyer's patches, lamina propria, and mesenteric nodes, were shown with anti-Ia monoclonal antibodies to be repopulated with recipient cells. This finding in grafts that appeared to be permanently accepted was surprising and contrary to expectations from the literature on intestinal allotransplantation.


Sujet(s)
Antibactériens/pharmacologie , Intestin grêle/transplantation , Transplantation/mortalité , Viscères/transplantation , Animaux , Poids , Immunohistochimie/méthodes , Immunosuppresseurs/pharmacologie , Intestin grêle/anatomopathologie , Mâle , Rats , Rats de lignée LEW , Lignées consanguines de rats , Coloration et marquage , Analyse de survie , Tacrolimus , Facteurs temps , Transplantation homologue
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