Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis

[Image: see text] Astatine-211 ((211)At) is an alpha emitter applicable to radioimmunotherapy (RIT), a cancer treatment that utilizes radioactive antibodies to target tumors. In the preparation of (211)At-labeled monoclonal antibodies ((211)At-mAbs), the possibility of radionuclide-induced antibody...

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Autores principales: Takashima, Hiroki, Ohnuki, Kazunobu, Manabe, Shino, Koga, Yoshikatsu, Tsumura, Ryo, Anzai, Takahiro, Wang, Yang, Yin, Xiaojie, Sato, Nozomi, Shigekawa, Yudai, Nambu, Akihiro, Usuda, Sachiko, Haba, Hiromitsu, Fujii, Hirofumi, Yasunaga, Masahiro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9906747/
https://www.ncbi.nlm.nih.gov/pubmed/36573995
http://dx.doi.org/10.1021/acs.molpharmaceut.2c00869
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author Takashima, Hiroki
Ohnuki, Kazunobu
Manabe, Shino
Koga, Yoshikatsu
Tsumura, Ryo
Anzai, Takahiro
Wang, Yang
Yin, Xiaojie
Sato, Nozomi
Shigekawa, Yudai
Nambu, Akihiro
Usuda, Sachiko
Haba, Hiromitsu
Fujii, Hirofumi
Yasunaga, Masahiro
author_facet Takashima, Hiroki
Ohnuki, Kazunobu
Manabe, Shino
Koga, Yoshikatsu
Tsumura, Ryo
Anzai, Takahiro
Wang, Yang
Yin, Xiaojie
Sato, Nozomi
Shigekawa, Yudai
Nambu, Akihiro
Usuda, Sachiko
Haba, Hiromitsu
Fujii, Hirofumi
Yasunaga, Masahiro
author_sort Takashima, Hiroki
collection PubMed
description [Image: see text] Astatine-211 ((211)At) is an alpha emitter applicable to radioimmunotherapy (RIT), a cancer treatment that utilizes radioactive antibodies to target tumors. In the preparation of (211)At-labeled monoclonal antibodies ((211)At-mAbs), the possibility of radionuclide-induced antibody denaturation (radiolysis) is of concern. Our previous study showed that this (211)At-induced radiochemical reaction disrupts the cellular binding activity of an astatinated mAb, resulting in attenuation of in vivo antitumor effects, whereas sodium ascorbate (SA), a free radical scavenger, prevents antibody denaturation, contributing to the maintenance of binding and antitumor activity. However, the influence of antibody denaturation on the pharmacokinetics of (211)At-mAbs relating to tumor accumulation, blood circulation time, and distribution to normal organs remains unclear. In this study, we use a radioactive anti-human epidermal growth factor receptor 2 (anti-HER2) mAb to demonstrate that an (211)At-induced radiochemical reaction disrupts active targeting via an antigen–antibody interaction, whereas SA helps to maintain targeting. In contrast, there was no difference in blood circulation time as well as distribution to normal organs between the stabilized and denatured immunoconjugates, indicating that antibody denaturation may not affect tumor accumulation via passive targeting based on the enhanced permeability and retention effect. In a high-HER2-expressing xenograft model treated with 1 MBq of (211)At-anti-HER2 mAbs, SA-dependent maintenance of active targeting contributed to a significantly better response. In treatment with 0.5 or 0.2 MBq, the stabilized radioactive mAb significantly reduced tumor growth compared to the denatured immunoconjugate. Additionally, through a comparison between a stabilized (211)At-anti-HER2 mAb and radioactive nontargeted control mAb, we demonstrate that active targeting significantly enhances tumor accumulation of radioactivity and in vivo antitumor effect. In RIT with (211)At, active targeting contributes to efficient tumor accumulation of radioactivity, resulting in a potent antitumor effect. SA-dependent protection that successfully maintains tumor targeting will facilitate the clinical application of alpha-RIT.
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spelling pubmed-99067472023-02-08 Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis Takashima, Hiroki Ohnuki, Kazunobu Manabe, Shino Koga, Yoshikatsu Tsumura, Ryo Anzai, Takahiro Wang, Yang Yin, Xiaojie Sato, Nozomi Shigekawa, Yudai Nambu, Akihiro Usuda, Sachiko Haba, Hiromitsu Fujii, Hirofumi Yasunaga, Masahiro Mol Pharm [Image: see text] Astatine-211 ((211)At) is an alpha emitter applicable to radioimmunotherapy (RIT), a cancer treatment that utilizes radioactive antibodies to target tumors. In the preparation of (211)At-labeled monoclonal antibodies ((211)At-mAbs), the possibility of radionuclide-induced antibody denaturation (radiolysis) is of concern. Our previous study showed that this (211)At-induced radiochemical reaction disrupts the cellular binding activity of an astatinated mAb, resulting in attenuation of in vivo antitumor effects, whereas sodium ascorbate (SA), a free radical scavenger, prevents antibody denaturation, contributing to the maintenance of binding and antitumor activity. However, the influence of antibody denaturation on the pharmacokinetics of (211)At-mAbs relating to tumor accumulation, blood circulation time, and distribution to normal organs remains unclear. In this study, we use a radioactive anti-human epidermal growth factor receptor 2 (anti-HER2) mAb to demonstrate that an (211)At-induced radiochemical reaction disrupts active targeting via an antigen–antibody interaction, whereas SA helps to maintain targeting. In contrast, there was no difference in blood circulation time as well as distribution to normal organs between the stabilized and denatured immunoconjugates, indicating that antibody denaturation may not affect tumor accumulation via passive targeting based on the enhanced permeability and retention effect. In a high-HER2-expressing xenograft model treated with 1 MBq of (211)At-anti-HER2 mAbs, SA-dependent maintenance of active targeting contributed to a significantly better response. In treatment with 0.5 or 0.2 MBq, the stabilized radioactive mAb significantly reduced tumor growth compared to the denatured immunoconjugate. Additionally, through a comparison between a stabilized (211)At-anti-HER2 mAb and radioactive nontargeted control mAb, we demonstrate that active targeting significantly enhances tumor accumulation of radioactivity and in vivo antitumor effect. In RIT with (211)At, active targeting contributes to efficient tumor accumulation of radioactivity, resulting in a potent antitumor effect. SA-dependent protection that successfully maintains tumor targeting will facilitate the clinical application of alpha-RIT. American Chemical Society 2022-12-27 /pmc/articles/PMC9906747/ /pubmed/36573995 http://dx.doi.org/10.1021/acs.molpharmaceut.2c00869 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by-nc-nd/4.0/Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Takashima, Hiroki
Ohnuki, Kazunobu
Manabe, Shino
Koga, Yoshikatsu
Tsumura, Ryo
Anzai, Takahiro
Wang, Yang
Yin, Xiaojie
Sato, Nozomi
Shigekawa, Yudai
Nambu, Akihiro
Usuda, Sachiko
Haba, Hiromitsu
Fujii, Hirofumi
Yasunaga, Masahiro
Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title_full Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title_fullStr Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title_full_unstemmed Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title_short Tumor Targeting of (211)At-Labeled Antibody under Sodium Ascorbate Protection against Radiolysis
title_sort tumor targeting of (211)at-labeled antibody under sodium ascorbate protection against radiolysis
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9906747/
https://www.ncbi.nlm.nih.gov/pubmed/36573995
http://dx.doi.org/10.1021/acs.molpharmaceut.2c00869
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