Positron Emission Tomography to Assess the Outcome of Intraportal Islet Transplantation

Author:

Eriksson Olof1,Selvaraju Ramkumar1,Eich Torsten2,Willny Mariam1,Brismar Torkel B.3,Carlbom Lina4,Ahlström Håkan4,Tufvesson Gunnar4,Lundgren Torbjörn5,Korsgren Olle2

Affiliation:

1. Preclinical PET Platform, Department of Medical Chemistry, Uppsala University, Uppsala, Sweden

2. Department of Immunology, Genetics and Pathology, Uppsala University, Uppsala, Sweden

3. Division of Medical Imaging and Technology, CLINTEC, Karolinska Institutet, Stockholm, Sweden

4. Department of Surgical Sciences, Uppsala University, Uppsala, Sweden

5. Division of Transplantation Surgery, CLINTEC, Karolinska Institutet, Stockholm, Sweden

Abstract

No imaging methodology currently exists to monitor viable islet mass after clinical intraportal islet transplantation. We investigated the potential of the endocrine positron emission tomography (PET) marker [11C]5-hydroxytryptophan ([11C]5-HTP) for this purpose. In a preclinical proof-of-concept study, the ex vivo and in vivo [11C]5-HTP signal was compared with the number of islets transplanted in rats. In a clinical study, human subjects with an intraportal islet graft (n = 8) underwent two [11C]5-HTP PET and MRI examinations 8 months apart. The tracer concentration in the liver as a whole, or in defined hotspots, was correlated to measurements of islet graft function. In rat, hepatic uptake of [11C]5-HTP correlated with the number of transplanted islets. In human subjects, uptake in hepatic hotspots showed a correlation with metabolic assessments of islet function. Change in hotspot standardized uptake value (SUV) predicted loss of graft function in one subject, whereas hotspot SUV was unchanged in subjects with stable graft function. The endocrine marker [11C]5-HTP thus shows a correlation between hepatic uptake and transplanted islet function and promise as a tool for noninvasive detection of viable islets. The evaluation procedure described can be used as a benchmark for novel agents targeting intraportally transplanted islets.

Funder

JDRF

National Institutes of Health

Swedish Medical Research Council

Barndiabetesfonden

Diabetesfonden

ExoDiab

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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