Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake

GLP-1 receptors are ideal targets for preoperative imaging of benign insulinoma and for quantifying the beta cell mass. The existing clinical tracers targeting GLP-1R are all agonists with low specific activity and very high kidney uptake. In order to solve those issues we evaluated GLP-1R agonist E...

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Autores principales: Läppchen, Tilman, Tönnesmann, Roswitha, Eersels, Jos, Meyer, Philipp T., Maecke, Helmut R., Rylova, Svetlana N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5245897/
https://www.ncbi.nlm.nih.gov/pubmed/28103285
http://dx.doi.org/10.1371/journal.pone.0170435
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author Läppchen, Tilman
Tönnesmann, Roswitha
Eersels, Jos
Meyer, Philipp T.
Maecke, Helmut R.
Rylova, Svetlana N.
author_facet Läppchen, Tilman
Tönnesmann, Roswitha
Eersels, Jos
Meyer, Philipp T.
Maecke, Helmut R.
Rylova, Svetlana N.
author_sort Läppchen, Tilman
collection PubMed
description GLP-1 receptors are ideal targets for preoperative imaging of benign insulinoma and for quantifying the beta cell mass. The existing clinical tracers targeting GLP-1R are all agonists with low specific activity and very high kidney uptake. In order to solve those issues we evaluated GLP-1R agonist Ex-4 and antagonist Ex(9–39) radioiodinated at Tyr(40) side by side with [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4 ((68)Ga-Ex-4) used in the clinic. The Kd, Bmax, internalization and binding kinetics of [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 and [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39) were studied in vitro using Ins-1E cells. Biodistribution and imaging studies were performed in nude mice bearing Ins-1E xenografts. In vitro evaluation demonstrated high affinity binding of the [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 agonist to the Ins-1E cells with fast internalization kinetics reaching a plateau after 30 min. The antagonist [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39) did not internalize and had a 4–fold higher K(d) value compared to the agonist. In contrast to [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39), which showed low and transient tumor uptake, [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 demonstrated excellent in vivo binding properties with tumor uptake identical to that of (68)Ga-Ex-4, but substantially lower kidney uptake resulting in a tumor-to-kidney ratio of 9.7 at 1 h compared to 0.3 with (68)Ga-Ex-4. Accumulation of activity in thyroid and stomach for both peptides, which was effectively blocked by irenat, confirms that in vivo deiodination is the mechanism behind the low kidney retention of iodinated peptides. The (124)I congener of [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 demonstrated a similar favourable biodistribution profile in the PET imaging studies in contrast to the typical biodistribution pattern of [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4. Our results demonstrate that iodinated Ex-4 is a very promising tracer for imaging of benign insulinomas. It solves the problem of high kidney uptake of the radiometal-labelled tracers by improving the tumor-to-kidney ratio measured for [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4 by 32 fold.
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spelling pubmed-52458972017-02-06 Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake Läppchen, Tilman Tönnesmann, Roswitha Eersels, Jos Meyer, Philipp T. Maecke, Helmut R. Rylova, Svetlana N. PLoS One Research Article GLP-1 receptors are ideal targets for preoperative imaging of benign insulinoma and for quantifying the beta cell mass. The existing clinical tracers targeting GLP-1R are all agonists with low specific activity and very high kidney uptake. In order to solve those issues we evaluated GLP-1R agonist Ex-4 and antagonist Ex(9–39) radioiodinated at Tyr(40) side by side with [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4 ((68)Ga-Ex-4) used in the clinic. The Kd, Bmax, internalization and binding kinetics of [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 and [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39) were studied in vitro using Ins-1E cells. Biodistribution and imaging studies were performed in nude mice bearing Ins-1E xenografts. In vitro evaluation demonstrated high affinity binding of the [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 agonist to the Ins-1E cells with fast internalization kinetics reaching a plateau after 30 min. The antagonist [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39) did not internalize and had a 4–fold higher K(d) value compared to the agonist. In contrast to [Nle(14),(125)I-Tyr(40)-NH(2)]Ex(9–39), which showed low and transient tumor uptake, [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 demonstrated excellent in vivo binding properties with tumor uptake identical to that of (68)Ga-Ex-4, but substantially lower kidney uptake resulting in a tumor-to-kidney ratio of 9.7 at 1 h compared to 0.3 with (68)Ga-Ex-4. Accumulation of activity in thyroid and stomach for both peptides, which was effectively blocked by irenat, confirms that in vivo deiodination is the mechanism behind the low kidney retention of iodinated peptides. The (124)I congener of [Nle(14),(125)I-Tyr(40)-NH(2)]Ex-4 demonstrated a similar favourable biodistribution profile in the PET imaging studies in contrast to the typical biodistribution pattern of [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4. Our results demonstrate that iodinated Ex-4 is a very promising tracer for imaging of benign insulinomas. It solves the problem of high kidney uptake of the radiometal-labelled tracers by improving the tumor-to-kidney ratio measured for [Nle(14),Lys(40)(Ahx-DOTA-(68)Ga)NH(2)]Ex-4 by 32 fold. Public Library of Science 2017-01-19 /pmc/articles/PMC5245897/ /pubmed/28103285 http://dx.doi.org/10.1371/journal.pone.0170435 Text en © 2017 Läppchen et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Läppchen, Tilman
Tönnesmann, Roswitha
Eersels, Jos
Meyer, Philipp T.
Maecke, Helmut R.
Rylova, Svetlana N.
Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title_full Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title_fullStr Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title_full_unstemmed Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title_short Radioiodinated Exendin-4 Is Superior to the Radiometal-Labelled Glucagon-Like Peptide-1 Receptor Probes Overcoming Their High Kidney Uptake
title_sort radioiodinated exendin-4 is superior to the radiometal-labelled glucagon-like peptide-1 receptor probes overcoming their high kidney uptake
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5245897/
https://www.ncbi.nlm.nih.gov/pubmed/28103285
http://dx.doi.org/10.1371/journal.pone.0170435
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