Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy

BACKGROUND: We recently reported a new absorbed dose conversion method, RAP (RAtio of Pharmacokinetics), for (211)At-meta-astatobenzylguanidine ((211)At-MABG) using a single biodistribution measurement, the percent injected dose/g. However, there were some mathematical ambiguities in determining the...

Descripción completa

Detalles Bibliográficos
Autores principales: Sakashita, Tetsuya, Matsumoto, Shojiro, Watanabe, Shigeki, Hanaoka, Hirofumi, Ohshima, Yasuhiro, Ikoma, Yoko, Ukon, Naoyuki, Sasaki, Ichiro, Higashi, Tatsuya, Higuchi, Tetsuya, Tsushima, Yoshito, Ishioka, Noriko S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer International Publishing 2021
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8665908/
https://www.ncbi.nlm.nih.gov/pubmed/34897556
http://dx.doi.org/10.1186/s40658-021-00425-z
_version_ 1784614106131595264
author Sakashita, Tetsuya
Matsumoto, Shojiro
Watanabe, Shigeki
Hanaoka, Hirofumi
Ohshima, Yasuhiro
Ikoma, Yoko
Ukon, Naoyuki
Sasaki, Ichiro
Higashi, Tatsuya
Higuchi, Tetsuya
Tsushima, Yoshito
Ishioka, Noriko S.
author_facet Sakashita, Tetsuya
Matsumoto, Shojiro
Watanabe, Shigeki
Hanaoka, Hirofumi
Ohshima, Yasuhiro
Ikoma, Yoko
Ukon, Naoyuki
Sasaki, Ichiro
Higashi, Tatsuya
Higuchi, Tetsuya
Tsushima, Yoshito
Ishioka, Noriko S.
author_sort Sakashita, Tetsuya
collection PubMed
description BACKGROUND: We recently reported a new absorbed dose conversion method, RAP (RAtio of Pharmacokinetics), for (211)At-meta-astatobenzylguanidine ((211)At-MABG) using a single biodistribution measurement, the percent injected dose/g. However, there were some mathematical ambiguities in determining the optimal timing of a single measurement of the percent injected dose/g. Thus, we aimed to mathematically reconstruct the RAP method and to examine the optimal timing of a single measurement. METHODS: We derived a new formalism of the RAP dose conversion method at time t. In addition, we acquired a formula to determine the optimal timing of a single measurement of the percent injected dose/g, assuming the one-compartment model for biological clearance. RESULTS: We investigated the new formalism’s performance using a representative RAP coefficient with radioactive decay weighting. Dose conversions by representative RAP coefficients predicted the true [(211)At]MABG absorbed doses with an error of 10% or less. The inverses of the representative RAP coefficients plotted at 4 h post-injection, which was the optimal timing reported in the previous work, were very close to the new inverses of the RAP coefficients 4 h post-injection. Next, the behavior of the optimal timing was analyzed by radiolabeled compounds with physical half-lives of 7.2 h and 10 d on various biological clearance half-lives. Behavior maps of optimal timing showed a tendency to converge to a constant value as the biological clearance half-life of a target increased. The areas of optimal timing for both compounds within a 5% or 10% prediction error were distributed around the optimal timing when the biological clearance half-life of a target was equal to that of the reference. Finally, an example of RAP dose conversion was demonstrated for [(211)At]MABG. CONCLUSIONS: The RAP dose conversion method renovated by the new formalism was able to estimate the [(211)At]MABG absorbed dose using a similar pharmacokinetics, such as [(131)I]MIBG. The present formalism revealed optimizing imaging time points on absorbed dose conversion between two radiopharmaceuticals. Further analysis and clinical data will be needed to elucidate the validity of a behavior map of the optimal timing of a single measurement for targeted alpha-nuclide therapy. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1186/s40658-021-00425-z.
format Online
Article
Text
id pubmed-8665908
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Springer International Publishing
record_format MEDLINE/PubMed
spelling pubmed-86659082021-12-27 Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy Sakashita, Tetsuya Matsumoto, Shojiro Watanabe, Shigeki Hanaoka, Hirofumi Ohshima, Yasuhiro Ikoma, Yoko Ukon, Naoyuki Sasaki, Ichiro Higashi, Tatsuya Higuchi, Tetsuya Tsushima, Yoshito Ishioka, Noriko S. EJNMMI Phys Original Research BACKGROUND: We recently reported a new absorbed dose conversion method, RAP (RAtio of Pharmacokinetics), for (211)At-meta-astatobenzylguanidine ((211)At-MABG) using a single biodistribution measurement, the percent injected dose/g. However, there were some mathematical ambiguities in determining the optimal timing of a single measurement of the percent injected dose/g. Thus, we aimed to mathematically reconstruct the RAP method and to examine the optimal timing of a single measurement. METHODS: We derived a new formalism of the RAP dose conversion method at time t. In addition, we acquired a formula to determine the optimal timing of a single measurement of the percent injected dose/g, assuming the one-compartment model for biological clearance. RESULTS: We investigated the new formalism’s performance using a representative RAP coefficient with radioactive decay weighting. Dose conversions by representative RAP coefficients predicted the true [(211)At]MABG absorbed doses with an error of 10% or less. The inverses of the representative RAP coefficients plotted at 4 h post-injection, which was the optimal timing reported in the previous work, were very close to the new inverses of the RAP coefficients 4 h post-injection. Next, the behavior of the optimal timing was analyzed by radiolabeled compounds with physical half-lives of 7.2 h and 10 d on various biological clearance half-lives. Behavior maps of optimal timing showed a tendency to converge to a constant value as the biological clearance half-life of a target increased. The areas of optimal timing for both compounds within a 5% or 10% prediction error were distributed around the optimal timing when the biological clearance half-life of a target was equal to that of the reference. Finally, an example of RAP dose conversion was demonstrated for [(211)At]MABG. CONCLUSIONS: The RAP dose conversion method renovated by the new formalism was able to estimate the [(211)At]MABG absorbed dose using a similar pharmacokinetics, such as [(131)I]MIBG. The present formalism revealed optimizing imaging time points on absorbed dose conversion between two radiopharmaceuticals. Further analysis and clinical data will be needed to elucidate the validity of a behavior map of the optimal timing of a single measurement for targeted alpha-nuclide therapy. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1186/s40658-021-00425-z. Springer International Publishing 2021-12-11 /pmc/articles/PMC8665908/ /pubmed/34897556 http://dx.doi.org/10.1186/s40658-021-00425-z Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/Open AccessThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Original Research
Sakashita, Tetsuya
Matsumoto, Shojiro
Watanabe, Shigeki
Hanaoka, Hirofumi
Ohshima, Yasuhiro
Ikoma, Yoko
Ukon, Naoyuki
Sasaki, Ichiro
Higashi, Tatsuya
Higuchi, Tetsuya
Tsushima, Yoshito
Ishioka, Noriko S.
Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title_full Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title_fullStr Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title_full_unstemmed Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title_short Nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
title_sort nonclinical study and applicability of the absorbed dose conversion method with a single biodistribution measurement for targeted alpha-nuclide therapy
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8665908/
https://www.ncbi.nlm.nih.gov/pubmed/34897556
http://dx.doi.org/10.1186/s40658-021-00425-z
work_keys_str_mv AT sakashitatetsuya nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT matsumotoshojiro nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT watanabeshigeki nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT hanaokahirofumi nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT ohshimayasuhiro nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT ikomayoko nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT ukonnaoyuki nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT sasakiichiro nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT higashitatsuya nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT higuchitetsuya nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT tsushimayoshito nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy
AT ishiokanorikos nonclinicalstudyandapplicabilityoftheabsorbeddoseconversionmethodwithasinglebiodistributionmeasurementfortargetedalphanuclidetherapy

Ejemplares similares