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System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations

BACKGROUND: (15)O-oxygen inhalation PET is unique in its ability to provide fundamental information regarding cerebral hemodynamics and energy metabolism in man. However, the use of (15)O-oxygen has been limited in a clinical environment largely attributed to logistical complexity, in relation to a...

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Autores principales: Iguchi, Satoshi, Moriguchi, Tetsuaki, Yamazaki, Makoto, Hori, Yuki, Koshino, Kazuhiro, Toyoda, Kazunori, Teuho, Jarmo, Shimochi, Saeka, Terakawa, Yusuke, Fukuda, Tetsuya, Takahashi, Jun C., Nakagawara, Jyoji, Kanaya, Shigehiko, Iida, Hidehiro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer International Publishing 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6300454/
https://www.ncbi.nlm.nih.gov/pubmed/30569426
http://dx.doi.org/10.1186/s40658-018-0236-5
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author Iguchi, Satoshi
Moriguchi, Tetsuaki
Yamazaki, Makoto
Hori, Yuki
Koshino, Kazuhiro
Toyoda, Kazunori
Teuho, Jarmo
Shimochi, Saeka
Terakawa, Yusuke
Fukuda, Tetsuya
Takahashi, Jun C.
Nakagawara, Jyoji
Kanaya, Shigehiko
Iida, Hidehiro
author_facet Iguchi, Satoshi
Moriguchi, Tetsuaki
Yamazaki, Makoto
Hori, Yuki
Koshino, Kazuhiro
Toyoda, Kazunori
Teuho, Jarmo
Shimochi, Saeka
Terakawa, Yusuke
Fukuda, Tetsuya
Takahashi, Jun C.
Nakagawara, Jyoji
Kanaya, Shigehiko
Iida, Hidehiro
author_sort Iguchi, Satoshi
collection PubMed
description BACKGROUND: (15)O-oxygen inhalation PET is unique in its ability to provide fundamental information regarding cerebral hemodynamics and energy metabolism in man. However, the use of (15)O-oxygen has been limited in a clinical environment largely attributed to logistical complexity, in relation to a long study period, and the need to produce and inhale three sets of radiopharmaceuticals. Despite the recent works that enabled shortening of the PET examination period, radiopharmaceutical production has still been a limiting factor. This study was aimed to evaluate a recently developed radiosynthesis/inhalation system that automatically supplies a series of (15)O-labeled gaseous radiopharmaceuticals of C(15)O, (15)O(2), and C(15)O(2) at short intervals. METHODS: The system consists of a radiosynthesizer which produces C(15)O, (15)O(2), and C(15)O(2); an inhalation controller; and an inhalation/scavenging unit. All three parts are controlled by a common sequencer, enabling automated production and inhalation at intervals less than 4.5 min. The gas inhalation/scavenging unit controls to sequentially supply of qualified radiopharmaceuticals at given radioactivity for given periods at given intervals. The unit also scavenges effectively the non-inhaled radioactive gases. Performance and reproducibility are evaluated. RESULTS: Using an (15)O-dedicated cyclotron with deuteron of 3.5 MeV at 40 μA, C(15)O, (15)O(2), and C(15)O(2) were sequentially produced at a constant rate of 1400, 2400, and 2000 MBq/min, respectively. Each of radiopharmaceuticals were stably inhaled at < 4.5 min intervals with negligible contamination from the previous supply. The two-hole two-layered face mask with scavenging device minimized the gaseous radioactivity surrounding subject’s face, while maintaining the normocapnia during examination periods. Quantitative assessment of net administration doses could be assessed using a pair of radio-detectors at inlet and scavenging tubes, as 541 ± 149, 320 ± 103, 523 ± 137 MBq corresponding to 2-min supply of 2574 ± 255 MBq for C(15)O, and 1-min supply of 2220 ± 766 and 1763 ± 174 for (15)O(2) and C(15)O(2), respectively. CONCLUSIONS: The present system allowed for automated production and inhalation of series of (15)O-labeled radiopharmaceuticals as required in the rapid (15)O-Oxygen PET protocol. The production and inhalation were reproducible and improved logistical complexity, and thus the use of (15)O-oxygen might have become practically applicable in clinical environments.
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spelling pubmed-63004542019-01-04 System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations Iguchi, Satoshi Moriguchi, Tetsuaki Yamazaki, Makoto Hori, Yuki Koshino, Kazuhiro Toyoda, Kazunori Teuho, Jarmo Shimochi, Saeka Terakawa, Yusuke Fukuda, Tetsuya Takahashi, Jun C. Nakagawara, Jyoji Kanaya, Shigehiko Iida, Hidehiro EJNMMI Phys Original Research BACKGROUND: (15)O-oxygen inhalation PET is unique in its ability to provide fundamental information regarding cerebral hemodynamics and energy metabolism in man. However, the use of (15)O-oxygen has been limited in a clinical environment largely attributed to logistical complexity, in relation to a long study period, and the need to produce and inhale three sets of radiopharmaceuticals. Despite the recent works that enabled shortening of the PET examination period, radiopharmaceutical production has still been a limiting factor. This study was aimed to evaluate a recently developed radiosynthesis/inhalation system that automatically supplies a series of (15)O-labeled gaseous radiopharmaceuticals of C(15)O, (15)O(2), and C(15)O(2) at short intervals. METHODS: The system consists of a radiosynthesizer which produces C(15)O, (15)O(2), and C(15)O(2); an inhalation controller; and an inhalation/scavenging unit. All three parts are controlled by a common sequencer, enabling automated production and inhalation at intervals less than 4.5 min. The gas inhalation/scavenging unit controls to sequentially supply of qualified radiopharmaceuticals at given radioactivity for given periods at given intervals. The unit also scavenges effectively the non-inhaled radioactive gases. Performance and reproducibility are evaluated. RESULTS: Using an (15)O-dedicated cyclotron with deuteron of 3.5 MeV at 40 μA, C(15)O, (15)O(2), and C(15)O(2) were sequentially produced at a constant rate of 1400, 2400, and 2000 MBq/min, respectively. Each of radiopharmaceuticals were stably inhaled at < 4.5 min intervals with negligible contamination from the previous supply. The two-hole two-layered face mask with scavenging device minimized the gaseous radioactivity surrounding subject’s face, while maintaining the normocapnia during examination periods. Quantitative assessment of net administration doses could be assessed using a pair of radio-detectors at inlet and scavenging tubes, as 541 ± 149, 320 ± 103, 523 ± 137 MBq corresponding to 2-min supply of 2574 ± 255 MBq for C(15)O, and 1-min supply of 2220 ± 766 and 1763 ± 174 for (15)O(2) and C(15)O(2), respectively. CONCLUSIONS: The present system allowed for automated production and inhalation of series of (15)O-labeled radiopharmaceuticals as required in the rapid (15)O-Oxygen PET protocol. The production and inhalation were reproducible and improved logistical complexity, and thus the use of (15)O-oxygen might have become practically applicable in clinical environments. Springer International Publishing 2018-12-19 /pmc/articles/PMC6300454/ /pubmed/30569426 http://dx.doi.org/10.1186/s40658-018-0236-5 Text en © The Author(s). 2018 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.
spellingShingle Original Research
Iguchi, Satoshi
Moriguchi, Tetsuaki
Yamazaki, Makoto
Hori, Yuki
Koshino, Kazuhiro
Toyoda, Kazunori
Teuho, Jarmo
Shimochi, Saeka
Terakawa, Yusuke
Fukuda, Tetsuya
Takahashi, Jun C.
Nakagawara, Jyoji
Kanaya, Shigehiko
Iida, Hidehiro
System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title_full System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title_fullStr System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title_full_unstemmed System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title_short System evaluation of automated production and inhalation of (15)O-labeled gaseous radiopharmaceuticals for the rapid (15)O-oxygen PET examinations
title_sort system evaluation of automated production and inhalation of (15)o-labeled gaseous radiopharmaceuticals for the rapid (15)o-oxygen pet examinations
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6300454/
https://www.ncbi.nlm.nih.gov/pubmed/30569426
http://dx.doi.org/10.1186/s40658-018-0236-5
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