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(American Journal of Pathology. 2001;158:745-755.)
© 2001 American Society for Investigative Pathology


Animal Model

A Transplantable Human Carcinoid as Model for Somatostatin Receptor-Mediated and Amine Transporter-Mediated Radionuclide Uptake

Lars Kölby*{dagger}, Peter Bernhardt{ddagger}, Håkan Ahlman*{dagger}, Bo Wängberg*{dagger}, Viktor Johanson*{dagger}, Annelie Wigander*{dagger}, Eva Forssell-Aronsson{ddagger}, Sven Karlsson§, Bo Ahrén§, Göran Stenman*{ddagger} and Ola Nilsson*{ddagger}

From The Lundberg Laboratory for Cancer Research,*
the Departments of Surgery,{dagger}
Pathology,{ddagger}
and Radiation Physics,{ddagger}
Sahlgrenska University Hospital, University of Göteberg, Göteberg; and the Department of Medicine,§
Malmö University Hospital, University of Lund, Malmö, Sweden

A human midgut carcinoid tumor was successfully transplanted into nude mice and propagated for five consecutive generations (30 months) with well-preserved phenotype. Tumor cells in nude mice expressed identical neuroendocrine markers as the original tumor, including somatostatin receptors (somatostatin receptors 1 to 5) and vesicular monoamine transporters (VMAT1 and VMAT2). Because of the expression of somatostatin receptors and VMAT1 and VMAT2 the grafted tumors could be visualized scintigraphically using the somatostatin analogue 111In-octreotide and the catecholamine analogue 123I-metaiodobenzylguanidine. The biokinetics of the somatostatin analogue 111In-octreotide in the tumors was studied and showed a high retention 7 days after administration. Cell cultures were re-established from transplanted tumors. Immunocytochemical and ultrastructural studies confirmed the neuroendocrine differentiation. The human origin of transplanted tumor cells was confirmed by cytogenetic and fluorescence it situ hybridization analyses. Spontaneous secretion of serotonin and its metabolite, 5-hydroxyindole acetic acid, from tumor cells was demonstrated. The tumor cells increased their [Ca2+]i in response to {beta}-adrenoceptor stimulation (isoproterenol) and K+-depolarization. All somatostatin receptor subtypes could be demonstrated in cultured cells. This human transplantable carcinoid tumor, designated GOT1, grafted to nude mice, will give unique possibilities for studies of somatostatin receptor- and VMAT-mediated radionuclide uptake as well as for studies of secretory mechanisms.





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