Islet cell function in long-term surviving primates after segmental pancreatic allotransplantation

Islet cell function was studied in pancreatectomized primates with functioning segmental pancreatic allografts more than 100 days after transplantation. Segmental allograft recipients were immunosuppresed with total lymphoid irradiation (TL1) and cyclosporine (CSA). After 100 days, islet function wa...

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Veröffentlicht in:Journal of surgical oncology 1988-05, Vol.38 (1), p.63-70, Article 63
Hauptverfasser: Du Toit, Don F., Heydenrych, Jacobus, Smit, Ben, Merwe, Emuel Van Der, Louw, Gabriel, Zuurmond, Theuns, Els, Daniel, Weideman, Andre, Toit, Lorraine Du, Wolfe-Coote, Sonja, Davids, Henry
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Sprache:eng
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Zusammenfassung:Islet cell function was studied in pancreatectomized primates with functioning segmental pancreatic allografts more than 100 days after transplantation. Segmental allograft recipients were immunosuppresed with total lymphoid irradiation (TL1) and cyclosporine (CSA). After 100 days, islet function was assessed, at which stage immunosuppression was terminated. Glucose, insulin, glucagon, and C‐peptide response was assessed during intravenous glucose tolerance test (IVGTT) and during arginine and tolbutamide stimulation. In eight normoglycaemic primates in which immunosuppressive treatment had been stopped and with mean graft survival of 145 days, islet stimulation was associated with moderate glucose intolerance, reduced K‐values, hypoinsulinaemia, and low C‐peptide values. Postmortem findings in all animals intentionally killed revealed severe graft atrophy in the absence of significant rejection. Severe graft atrophy in normoglycaemic primates, together with significantly impaired graft function after segmental pancreatic transplantation compared to normal animals, suggest that transplantation of the whole pancreas may be mandatory if normal or near‐normal function is to be achieved.
ISSN:0022-4790
1096-9098
DOI:10.1002/jso.2930380116