Islet Graft Assessment in the Edmonton Protocol

Author:

Street Cale N.1,Lakey Jonathan R.T.12,Shapiro A.M. James12,Imes Sharleen3,Rajotte Ray V.124,Ryan Edmond A.4,Lyon James G.1,Kin Tatsuya1,Avila Jose1,Tsujimura Toshiaki1,Korbutt Gregory S.125

Affiliation:

1. Surgical-Medical Research Institute, University of Alberta, Edmonton, Alberta, Canada

2. Department of Surgery, University of Alberta, Edmonton, Alberta, Canada

3. Capital Health Authority, Edmonton, Alberta, Canada

4. Department of Medicine, University of Alberta, Edmonton, Alberta, Canada

5. Stem Cell Network of Canada, Ottawa, Ontario, Canada

Abstract

The success of the Edmonton Protocol for islet transplantation has provided new hope in the treatment of type 1 diabetes. This study reports on the assessment of 83 human islet grafts transplanted using the Edmonton Protocol since 1999. Cellular composition, as assessed by immunohistochemistry, showed a lower islet purity (∼40%) than has been reported in previous studies using dithizone staining to quantitate islet equivalents. Furthermore, grafts were found to contain substantial populations of exocrine and ductal tissue. Total cellular insulin transplanted was 8,097.6 ± 3,164.4 μg/patient, and was significantly lower in bottom gradient layer grafts than top gradient layer or whole/combined grafts (P < 0.0005). A static incubation test for islet function gave a stimulation index of 3–4, although this measure did not correlate with posttransplant metabolic outcome. Furthermore, we confirmed a previously reported trend in which donor age affects islet yield and purity. It is important to note that a significant positive correlation was observed between the number of islet progenitor (ductal-epithelial) cells transplanted and long-term metabolic success as assessed an by intravenous glucose tolerance test at ∼2 years posttransplant. In summary, careful assessment of islet graft composition is needed in a clinical transplantation program to accurately estimate islet purity and assess the contribution of other cell types present, such as islet progenitor cells.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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