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Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study

(1) Background: Theranostic approaches in the management of cholecystokinin subtype 2 receptor (CCK(2)R)-positive tumors include radiolabeled gastrin and CCK motifs. Moving toward antagonist-based CCK(2)R-radioligands instead, we herein present three analogs of the nonpeptidic CCK(2)R-antagonist Z36...

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Autores principales: Nock, Berthold A., Kanellopoulos, Panagiotis, Chepurny, Oleg G., Rouchota, Maritina, Loudos, George, Holz, George G., Krenning, Eric P., Maina, Theodosia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8954547/
https://www.ncbi.nlm.nih.gov/pubmed/35336041
http://dx.doi.org/10.3390/pharmaceutics14030666
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author Nock, Berthold A.
Kanellopoulos, Panagiotis
Chepurny, Oleg G.
Rouchota, Maritina
Loudos, George
Holz, George G.
Krenning, Eric P.
Maina, Theodosia
author_facet Nock, Berthold A.
Kanellopoulos, Panagiotis
Chepurny, Oleg G.
Rouchota, Maritina
Loudos, George
Holz, George G.
Krenning, Eric P.
Maina, Theodosia
author_sort Nock, Berthold A.
collection PubMed
description (1) Background: Theranostic approaches in the management of cholecystokinin subtype 2 receptor (CCK(2)R)-positive tumors include radiolabeled gastrin and CCK motifs. Moving toward antagonist-based CCK(2)R-radioligands instead, we herein present three analogs of the nonpeptidic CCK(2)R-antagonist Z360, GAS1/2/3. Each was conjugated to a different chelator (DOTA, NODAGA or DOTAGA) for labeling with medically relevant trivalent radiometals (e.g., Ga-68, In-111, Lu-177) for potential use as anti-CCK(2)R cancer agents; (2) Methods: The in vitro properties of the thee analogs were compared in stably transfected HEK293-CCK(2)R cells. Biodistribution profiles were compared in SCID mice bearing twin HEK293-CCK(2)R and wtHEK293 tumors; (3) Results: The GAS1/2/3 analogs displayed high CCK(2)R-affinity (lower nM-range). The radioligands were fairly stable in vivo and selectively targeted the HEK293-CCK(2)R, but not the CCK(2)R-negative wtHEK293 tumors in mice. Their overall pharmacokinetic profile was found strongly dependent on the radiometal-chelate. Results could be visualized by SPECT/CT for the [(111)In]In-analogs; (4) Conclusions: The present study highlighted the high impact of the radiometal-chelate on the end-pharmacokinetics of a new series of Z360-based radioligands, revealing candidates with promising properties for clinical translation. It also provided the impetus for the development of a new class of nonpeptidic radioligands for CCK(2)R-targeted theranostics of human cancer.
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spelling pubmed-89545472022-03-26 Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study Nock, Berthold A. Kanellopoulos, Panagiotis Chepurny, Oleg G. Rouchota, Maritina Loudos, George Holz, George G. Krenning, Eric P. Maina, Theodosia Pharmaceutics Article (1) Background: Theranostic approaches in the management of cholecystokinin subtype 2 receptor (CCK(2)R)-positive tumors include radiolabeled gastrin and CCK motifs. Moving toward antagonist-based CCK(2)R-radioligands instead, we herein present three analogs of the nonpeptidic CCK(2)R-antagonist Z360, GAS1/2/3. Each was conjugated to a different chelator (DOTA, NODAGA or DOTAGA) for labeling with medically relevant trivalent radiometals (e.g., Ga-68, In-111, Lu-177) for potential use as anti-CCK(2)R cancer agents; (2) Methods: The in vitro properties of the thee analogs were compared in stably transfected HEK293-CCK(2)R cells. Biodistribution profiles were compared in SCID mice bearing twin HEK293-CCK(2)R and wtHEK293 tumors; (3) Results: The GAS1/2/3 analogs displayed high CCK(2)R-affinity (lower nM-range). The radioligands were fairly stable in vivo and selectively targeted the HEK293-CCK(2)R, but not the CCK(2)R-negative wtHEK293 tumors in mice. Their overall pharmacokinetic profile was found strongly dependent on the radiometal-chelate. Results could be visualized by SPECT/CT for the [(111)In]In-analogs; (4) Conclusions: The present study highlighted the high impact of the radiometal-chelate on the end-pharmacokinetics of a new series of Z360-based radioligands, revealing candidates with promising properties for clinical translation. It also provided the impetus for the development of a new class of nonpeptidic radioligands for CCK(2)R-targeted theranostics of human cancer. MDPI 2022-03-18 /pmc/articles/PMC8954547/ /pubmed/35336041 http://dx.doi.org/10.3390/pharmaceutics14030666 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Nock, Berthold A.
Kanellopoulos, Panagiotis
Chepurny, Oleg G.
Rouchota, Maritina
Loudos, George
Holz, George G.
Krenning, Eric P.
Maina, Theodosia
Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title_full Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title_fullStr Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title_full_unstemmed Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title_short Nonpeptidic Z360-Analogs Tagged with Trivalent Radiometals as Anti-CCK(2)R Cancer Theranostic Agents: A Preclinical Study
title_sort nonpeptidic z360-analogs tagged with trivalent radiometals as anti-cck(2)r cancer theranostic agents: a preclinical study
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8954547/
https://www.ncbi.nlm.nih.gov/pubmed/35336041
http://dx.doi.org/10.3390/pharmaceutics14030666
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