Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study

OBJECTIVE(S): It is difficult to investigate the whole-body distribution of an orally administered drug by means of positron emission tomography (PET), owing to the short physical half-life of radionuclides, especially when (11)C-labeled compounds are tested. Therefore, we aimed to examine the whole...

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Autores principales: Mochida, Ikuko, Shimosegawa, Eku, Kanai, Yasukazu, Naka, Sadahiro, Matsunaga, Keiko, Isohashi, Kayako, Horitsugi, Genki, Watabe, Tadashi, Kato, Hiroki, Hatazawa, Jun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Asia Oceania Journal of Nuclear Medicine & Biology 2017
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Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5221682/
https://www.ncbi.nlm.nih.gov/pubmed/28840133
http://dx.doi.org/10.22038/aojnmb.2016.7513
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author Mochida, Ikuko
Shimosegawa, Eku
Kanai, Yasukazu
Naka, Sadahiro
Matsunaga, Keiko
Isohashi, Kayako
Horitsugi, Genki
Watabe, Tadashi
Kato, Hiroki
Hatazawa, Jun
author_facet Mochida, Ikuko
Shimosegawa, Eku
Kanai, Yasukazu
Naka, Sadahiro
Matsunaga, Keiko
Isohashi, Kayako
Horitsugi, Genki
Watabe, Tadashi
Kato, Hiroki
Hatazawa, Jun
author_sort Mochida, Ikuko
collection PubMed
description OBJECTIVE(S): It is difficult to investigate the whole-body distribution of an orally administered drug by means of positron emission tomography (PET), owing to the short physical half-life of radionuclides, especially when (11)C-labeled compounds are tested. Therefore, we aimed to examine the whole-body distribution of donepezil (DNP) as an acetylcholinesterase inhibitor by means of (11)C-DNP PET imaging, combined with the oral administration of pharmacological doses of DNP. METHODS: We studied 14 healthy volunteers, divided into group A (n=4) and group B (n=10). At first, we studied four females (mean age: 57.3±4.5 y), three of whom underwent (11)C-DNP PET scan at 2.5 h after the oral administration of 1 mg and 30 µg of DNP, respectively, while one patient was scanned following the oral administration of 30 µg of DNP (group A). Then, we studied five females and five males (48.3±6.1 y), who underwent (11)C-DNP PET scan, without the oral administration of DNP (group B). Plasma DNP concentration upon scanning was measured by tandem mass spectrometry. Arterialized venous blood samples were collected periodically to measure plasma radioactivity and metabolites. In group A, (11)C-DNP PET scan of the brain and whole body continued for 60 and 20 min, respectively. Subjects in group B underwent sequential whole-body scan for 60 min. The regional uptake of (11)C-DNP was analyzed by measuring the standard uptake value (SUV) through setting regions of interest on major organs with reference CT. RESULTS: In group A, plasma DNP concentration was significantly correlated with the orally administered dose of DNP. The mean plasma concentration was 2.00 nM (n=3) after 1 mg oral administration and 0.06 nM (n=4) after 30 µg oral administration. No significant difference in plasma radioactivity or fraction of metabolites was found between groups A and B. High (11)C-DNP accumulation was found in the liver, stomach, pancreas, brain, salivary glands, bone marrow, and myocardium in groups A and B, in this order. No significant difference in SUV value was found among (11)C-DNP PET studies after the oral administration of 1 mg of DNP, 30 µg of DNP, or no DNP. CONCLUSION: The present study demonstrated that the whole-body distribution of DNP after the oral administration of pharmacological doses could be evaluated by (11)C-DNP PET studies, combined with the oral administration of DNP.
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spelling pubmed-52216822017-08-24 Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study Mochida, Ikuko Shimosegawa, Eku Kanai, Yasukazu Naka, Sadahiro Matsunaga, Keiko Isohashi, Kayako Horitsugi, Genki Watabe, Tadashi Kato, Hiroki Hatazawa, Jun Asia Ocean J Nucl Med Biol Original Article OBJECTIVE(S): It is difficult to investigate the whole-body distribution of an orally administered drug by means of positron emission tomography (PET), owing to the short physical half-life of radionuclides, especially when (11)C-labeled compounds are tested. Therefore, we aimed to examine the whole-body distribution of donepezil (DNP) as an acetylcholinesterase inhibitor by means of (11)C-DNP PET imaging, combined with the oral administration of pharmacological doses of DNP. METHODS: We studied 14 healthy volunteers, divided into group A (n=4) and group B (n=10). At first, we studied four females (mean age: 57.3±4.5 y), three of whom underwent (11)C-DNP PET scan at 2.5 h after the oral administration of 1 mg and 30 µg of DNP, respectively, while one patient was scanned following the oral administration of 30 µg of DNP (group A). Then, we studied five females and five males (48.3±6.1 y), who underwent (11)C-DNP PET scan, without the oral administration of DNP (group B). Plasma DNP concentration upon scanning was measured by tandem mass spectrometry. Arterialized venous blood samples were collected periodically to measure plasma radioactivity and metabolites. In group A, (11)C-DNP PET scan of the brain and whole body continued for 60 and 20 min, respectively. Subjects in group B underwent sequential whole-body scan for 60 min. The regional uptake of (11)C-DNP was analyzed by measuring the standard uptake value (SUV) through setting regions of interest on major organs with reference CT. RESULTS: In group A, plasma DNP concentration was significantly correlated with the orally administered dose of DNP. The mean plasma concentration was 2.00 nM (n=3) after 1 mg oral administration and 0.06 nM (n=4) after 30 µg oral administration. No significant difference in plasma radioactivity or fraction of metabolites was found between groups A and B. High (11)C-DNP accumulation was found in the liver, stomach, pancreas, brain, salivary glands, bone marrow, and myocardium in groups A and B, in this order. No significant difference in SUV value was found among (11)C-DNP PET studies after the oral administration of 1 mg of DNP, 30 µg of DNP, or no DNP. CONCLUSION: The present study demonstrated that the whole-body distribution of DNP after the oral administration of pharmacological doses could be evaluated by (11)C-DNP PET studies, combined with the oral administration of DNP. Asia Oceania Journal of Nuclear Medicine & Biology 2017 /pmc/articles/PMC5221682/ /pubmed/28840133 http://dx.doi.org/10.22038/aojnmb.2016.7513 Text en Copyright: © 2017 mums.ac.ir http://creativecommons.org/licenses/by/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Article
Mochida, Ikuko
Shimosegawa, Eku
Kanai, Yasukazu
Naka, Sadahiro
Matsunaga, Keiko
Isohashi, Kayako
Horitsugi, Genki
Watabe, Tadashi
Kato, Hiroki
Hatazawa, Jun
Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title_full Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title_fullStr Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title_full_unstemmed Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title_short Whole-Body Distribution of Donepezil as an Acetylcholinesterase Inhibitor after Oral Administration in Normal Human Subjects: A (11)C-donepezil PET Study
title_sort whole-body distribution of donepezil as an acetylcholinesterase inhibitor after oral administration in normal human subjects: a (11)c-donepezil pet study
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5221682/
https://www.ncbi.nlm.nih.gov/pubmed/28840133
http://dx.doi.org/10.22038/aojnmb.2016.7513
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