The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model

Copper-64 is an attractive radionuclide for PET imaging and is frequently used in clinical applications. The aim of this study was to perform a side-by-side comparison of the in vitro and in vivo performance of (64)Cu-NODAGA-JR11 (NODAGA = 1,4,7-triazacyclononane,1-glutaric acid,4,7-acetic acid, JR1...

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Autores principales: Rylova, Svetlana N., Stoykow, Christian, Del Pozzo, Luigi, Abiraj, Keelara, Tamma, Maria Luisa, Kiefer, Yvonne, Fani, Melpomeni, Maecke, Helmut R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5906006/
https://www.ncbi.nlm.nih.gov/pubmed/29668724
http://dx.doi.org/10.1371/journal.pone.0195802
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author Rylova, Svetlana N.
Stoykow, Christian
Del Pozzo, Luigi
Abiraj, Keelara
Tamma, Maria Luisa
Kiefer, Yvonne
Fani, Melpomeni
Maecke, Helmut R.
author_facet Rylova, Svetlana N.
Stoykow, Christian
Del Pozzo, Luigi
Abiraj, Keelara
Tamma, Maria Luisa
Kiefer, Yvonne
Fani, Melpomeni
Maecke, Helmut R.
author_sort Rylova, Svetlana N.
collection PubMed
description Copper-64 is an attractive radionuclide for PET imaging and is frequently used in clinical applications. The aim of this study was to perform a side-by-side comparison of the in vitro and in vivo performance of (64)Cu-NODAGA-JR11 (NODAGA = 1,4,7-triazacyclononane,1-glutaric acid,4,7-acetic acid, JR11 = p-Cl-Phe-cyclo(D-Cys-Aph(Hor)-D-Aph(cbm)-Lys-Thr-Cys)D-Tyr-NH(2)), a somatostatin receptor 2 antagonist, with the clinically used sst2 agonist (64)Cu-DOTA-TATE ((TATE = D-Phe-cyclo(Cys-Tyr-D-Trp-Lys-Thr-Cys)Thr). In vitro studies demonstrated K(d) values of 5.7±0.95 nM (Bmax = 4.1±0.18 nM) for the antagonist (64/nat)Cu-NODAGA-JR11 and 20.1±4.4. nM (Bmax = 0.48±0.18 nM) for the agonist (64/nat)Cu-DOTA-TATE. Cell uptake studies showed the expected differences between agonists and antagonists. Whereas (64)Cu-DOTA-TATE (the agonist) showed very effective internalization in the cell culture assay (with 50% internalized at 4 hours post-peptide addition under the given experimental conditions), (64)Cu-NODAGA-JR11 (the antagonist) showed little internalization but strong receptor-mediated uptake at the cell membrane. Biodistribution studies of (64)Cu-NODAGA-JR11 showed rapid blood clearance and tumor uptake with increasing tumor-to-relevant organ ratios within the first 4 hours and in some cases, 24 hours, respectively. The tumor washout was slow or non-existent in the first 4 hours, whereas the kidney washout was very efficient, leading to high and increasing tumor-to-kidney ratios over time. Specificity of tumor uptake was proven by co-injection of high excess of non-radiolabeled peptide, which led to >80% tumor blocking. (64)Cu-DOTA-TATE showed less favorable pharmacokinetics, with the exception of lower kidney uptake. Blood clearance was distinctly slower and persistent higher blood values were found at 24 hours. Uptake in the liver and lung was relatively high and also persistent. The tumor uptake was specific and similar to that of (64)Cu-NODAGA-JR11 at 1 h, but release from the tumor was very fast, particularly between 4 and 24 hours. Tumor-to-normal organ ratios were distinctly lower after 1 hour. This is indicative of insufficient in vivo stability. PET studies of (64)Cu-NODAGA-JR11 reflected the biodistribution data with nicely delineated tumor and low background. (64)Cu-NODAGA-JR11 shows promising pharmacokinetic properties for further translation into the clinic.
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spelling pubmed-59060062018-05-06 The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model Rylova, Svetlana N. Stoykow, Christian Del Pozzo, Luigi Abiraj, Keelara Tamma, Maria Luisa Kiefer, Yvonne Fani, Melpomeni Maecke, Helmut R. PLoS One Research Article Copper-64 is an attractive radionuclide for PET imaging and is frequently used in clinical applications. The aim of this study was to perform a side-by-side comparison of the in vitro and in vivo performance of (64)Cu-NODAGA-JR11 (NODAGA = 1,4,7-triazacyclononane,1-glutaric acid,4,7-acetic acid, JR11 = p-Cl-Phe-cyclo(D-Cys-Aph(Hor)-D-Aph(cbm)-Lys-Thr-Cys)D-Tyr-NH(2)), a somatostatin receptor 2 antagonist, with the clinically used sst2 agonist (64)Cu-DOTA-TATE ((TATE = D-Phe-cyclo(Cys-Tyr-D-Trp-Lys-Thr-Cys)Thr). In vitro studies demonstrated K(d) values of 5.7±0.95 nM (Bmax = 4.1±0.18 nM) for the antagonist (64/nat)Cu-NODAGA-JR11 and 20.1±4.4. nM (Bmax = 0.48±0.18 nM) for the agonist (64/nat)Cu-DOTA-TATE. Cell uptake studies showed the expected differences between agonists and antagonists. Whereas (64)Cu-DOTA-TATE (the agonist) showed very effective internalization in the cell culture assay (with 50% internalized at 4 hours post-peptide addition under the given experimental conditions), (64)Cu-NODAGA-JR11 (the antagonist) showed little internalization but strong receptor-mediated uptake at the cell membrane. Biodistribution studies of (64)Cu-NODAGA-JR11 showed rapid blood clearance and tumor uptake with increasing tumor-to-relevant organ ratios within the first 4 hours and in some cases, 24 hours, respectively. The tumor washout was slow or non-existent in the first 4 hours, whereas the kidney washout was very efficient, leading to high and increasing tumor-to-kidney ratios over time. Specificity of tumor uptake was proven by co-injection of high excess of non-radiolabeled peptide, which led to >80% tumor blocking. (64)Cu-DOTA-TATE showed less favorable pharmacokinetics, with the exception of lower kidney uptake. Blood clearance was distinctly slower and persistent higher blood values were found at 24 hours. Uptake in the liver and lung was relatively high and also persistent. The tumor uptake was specific and similar to that of (64)Cu-NODAGA-JR11 at 1 h, but release from the tumor was very fast, particularly between 4 and 24 hours. Tumor-to-normal organ ratios were distinctly lower after 1 hour. This is indicative of insufficient in vivo stability. PET studies of (64)Cu-NODAGA-JR11 reflected the biodistribution data with nicely delineated tumor and low background. (64)Cu-NODAGA-JR11 shows promising pharmacokinetic properties for further translation into the clinic. Public Library of Science 2018-04-18 /pmc/articles/PMC5906006/ /pubmed/29668724 http://dx.doi.org/10.1371/journal.pone.0195802 Text en © 2018 Rylova 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
Rylova, Svetlana N.
Stoykow, Christian
Del Pozzo, Luigi
Abiraj, Keelara
Tamma, Maria Luisa
Kiefer, Yvonne
Fani, Melpomeni
Maecke, Helmut R.
The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title_full The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title_fullStr The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title_full_unstemmed The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title_short The somatostatin receptor 2 antagonist (64)Cu-NODAGA-JR11 outperforms (64)Cu-DOTA-TATE in a mouse xenograft model
title_sort somatostatin receptor 2 antagonist (64)cu-nodaga-jr11 outperforms (64)cu-dota-tate in a mouse xenograft model
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5906006/
https://www.ncbi.nlm.nih.gov/pubmed/29668724
http://dx.doi.org/10.1371/journal.pone.0195802
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