Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate

P-cadherin is overexpressed in various cancers and can be a target for radioimmunotherapy. We investigated the preclinical pharmacokinetics and pharmacology of FF-21101, an (111)In- or (90)Y-conjugated monoclonal antibody against P-cadherin, to evaluate its clinical applications. Methods: The radioc...

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Autores principales: Funase, Yuichi, Nakamura, Eri, Kajita, Masamichi, Saito, Yasutaka, Oshikiri, Shinobu, Kitano, Michi, Tokura, Masahiko, Hino, Akihiro, Uehara, Tomoya
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society of Nuclear Medicine 2021
Materias:
Theranostics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8679590/
https://www.ncbi.nlm.nih.gov/pubmed/32737245
http://dx.doi.org/10.2967/jnumed.120.245837
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author Funase, Yuichi
Nakamura, Eri
Kajita, Masamichi
Saito, Yasutaka
Oshikiri, Shinobu
Kitano, Michi
Tokura, Masahiko
Hino, Akihiro
Uehara, Tomoya
author_facet Funase, Yuichi
Nakamura, Eri
Kajita, Masamichi
Saito, Yasutaka
Oshikiri, Shinobu
Kitano, Michi
Tokura, Masahiko
Hino, Akihiro
Uehara, Tomoya
author_sort Funase, Yuichi
collection PubMed
description P-cadherin is overexpressed in various cancers and can be a target for radioimmunotherapy. We investigated the preclinical pharmacokinetics and pharmacology of FF-21101, an (111)In- or (90)Y-conjugated monoclonal antibody against P-cadherin, to evaluate its clinical applications. Methods: The radiochemical purity, binding affinity, and in vitro serum stability of (111)In or (90)Y-labeled FF-21101 were evaluated. The pharmacokinetics of (111)In or (90)Y-FF-21101 were compared in normal mice. Tumor accumulation after (111)In-FF-21101 administration was investigated in mice bearing subcutaneous tumors with high (NCI-H1373), moderate (EBC-1), or no (A549) P-cadherin expression. The tumor suppression effect after a single intravenous injection of (90)Y-FF-21101 was assessed in NCI-H1373 and EBC-1 mouse xenograft models. The relationship between antibody dose and tumor accumulation was investigated in the NCI-H1373 mouse xenograft model. The absorbed radiation dose in humans after injection of (90)Y-FF-21101 was estimated using γ-camera images of cynomolgus monkeys. Results: The radiochemical purities of (111)In- and (90)Y-FF-21101 were 98.2% ± 2.5% (n = 9) and 99.3% ± 0.6% (n = 5), respectively. The dissociation constants were 1.083 nM for (111)In-FF-21101 and 1.367 nM for (90)Y-FF-21101. Both (111)In- and (90)Y-FF-21101 were stable in human serum after 96 h of incubation and exhibited similar pharmacokinetics in normal mice. The tumor accumulation of (111)In-FF-21101 was closely related to the intensity of P-cadherin expression in the cells. (90)Y-FF-21101 showed significant tumor growth inhibition, indicating that NCI-H1373 and EBC-1 recurrence was not observed after intravenous administration of 3.7 and 7.4 MBq, respectively of (90)Y-FF-21101 per animal. Tumor uptake in the mouse xenograft model and estimated absorbed radiation doses in the spleen of monkeys decreased with increasing antibody doses of (111)In-FF-21101. Conversely, the estimated absorbed radiation dose in the red marrow increased with increasing antibody dose. An antibody dose of 4.8 mg/m(2) was considered appropriate for humans, on the basis of efficacy and safety. The maximum tolerated administered activity of (90)Y-FF-21101 was estimated to be 2,886 MBq/human. Conclusion: FF-21101 radioimmunotherapy exhibited high antitumor affinity and antitumor efficacy in mouse xenograft models. Extrapolation of the pharmacokinetics in monkeys to humans suggests the potential for clinical application of FF-21101 for treating P-cadherin–expressing tumor.
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spelling pubmed-86795902022-01-21 Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate Funase, Yuichi Nakamura, Eri Kajita, Masamichi Saito, Yasutaka Oshikiri, Shinobu Kitano, Michi Tokura, Masahiko Hino, Akihiro Uehara, Tomoya J Nucl Med Theranostics P-cadherin is overexpressed in various cancers and can be a target for radioimmunotherapy. We investigated the preclinical pharmacokinetics and pharmacology of FF-21101, an (111)In- or (90)Y-conjugated monoclonal antibody against P-cadherin, to evaluate its clinical applications. Methods: The radiochemical purity, binding affinity, and in vitro serum stability of (111)In or (90)Y-labeled FF-21101 were evaluated. The pharmacokinetics of (111)In or (90)Y-FF-21101 were compared in normal mice. Tumor accumulation after (111)In-FF-21101 administration was investigated in mice bearing subcutaneous tumors with high (NCI-H1373), moderate (EBC-1), or no (A549) P-cadherin expression. The tumor suppression effect after a single intravenous injection of (90)Y-FF-21101 was assessed in NCI-H1373 and EBC-1 mouse xenograft models. The relationship between antibody dose and tumor accumulation was investigated in the NCI-H1373 mouse xenograft model. The absorbed radiation dose in humans after injection of (90)Y-FF-21101 was estimated using γ-camera images of cynomolgus monkeys. Results: The radiochemical purities of (111)In- and (90)Y-FF-21101 were 98.2% ± 2.5% (n = 9) and 99.3% ± 0.6% (n = 5), respectively. The dissociation constants were 1.083 nM for (111)In-FF-21101 and 1.367 nM for (90)Y-FF-21101. Both (111)In- and (90)Y-FF-21101 were stable in human serum after 96 h of incubation and exhibited similar pharmacokinetics in normal mice. The tumor accumulation of (111)In-FF-21101 was closely related to the intensity of P-cadherin expression in the cells. (90)Y-FF-21101 showed significant tumor growth inhibition, indicating that NCI-H1373 and EBC-1 recurrence was not observed after intravenous administration of 3.7 and 7.4 MBq, respectively of (90)Y-FF-21101 per animal. Tumor uptake in the mouse xenograft model and estimated absorbed radiation doses in the spleen of monkeys decreased with increasing antibody doses of (111)In-FF-21101. Conversely, the estimated absorbed radiation dose in the red marrow increased with increasing antibody dose. An antibody dose of 4.8 mg/m(2) was considered appropriate for humans, on the basis of efficacy and safety. The maximum tolerated administered activity of (90)Y-FF-21101 was estimated to be 2,886 MBq/human. Conclusion: FF-21101 radioimmunotherapy exhibited high antitumor affinity and antitumor efficacy in mouse xenograft models. Extrapolation of the pharmacokinetics in monkeys to humans suggests the potential for clinical application of FF-21101 for treating P-cadherin–expressing tumor. Society of Nuclear Medicine 2021-02 /pmc/articles/PMC8679590/ /pubmed/32737245 http://dx.doi.org/10.2967/jnumed.120.245837 Text en © 2021 by the Society of Nuclear Medicine and Molecular Imaging. https://creativecommons.org/licenses/by/4.0/Immediate Open Access: Creative Commons Attribution 4.0 International License (CC BY) allows users to share and adapt with attribution, excluding materials credited to previous publications. License: https://creativecommons.org/licenses/by/4.0/. Details: http://jnm.snmjournals.org/site/misc/permission.xhtml.
spellingShingle Theranostics
Funase, Yuichi
Nakamura, Eri
Kajita, Masamichi
Saito, Yasutaka
Oshikiri, Shinobu
Kitano, Michi
Tokura, Masahiko
Hino, Akihiro
Uehara, Tomoya
Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title_full Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title_fullStr Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title_full_unstemmed Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title_short Preclinical Characterization of the Radioimmunoconjugate (111)In or (90)Y-FF-21101 Against a P-Cadherin–Expressing Tumor in a Mouse Xenograft Model and a Nonhuman Primate
title_sort preclinical characterization of the radioimmunoconjugate (111)in or (90)y-ff-21101 against a p-cadherin–expressing tumor in a mouse xenograft model and a nonhuman primate
topic Theranostics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8679590/
https://www.ncbi.nlm.nih.gov/pubmed/32737245
http://dx.doi.org/10.2967/jnumed.120.245837
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