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Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model

Although acotiamide hydrochloride hydrate (acotiamide-HH) has not been reported to have genotoxic findings in any of the genotoxicity studies or treatment-related toxicological findings in reproductive and developmental studies, suspicious uterine tumorigenesis was observed in the results of a long-...

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Autores principales: Kuroda, Hiroyuki, Kinomoto, Toshiko, Ogawa, Shuji, Kawabe, Mayumi, Suguro, Mayuko, Naraoka, Hitoshi, Takamatsu, Kazuhiko, Oishi, Yuji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Japanese Society of Toxicologic Pathology 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5820101/
https://www.ncbi.nlm.nih.gov/pubmed/29479138
http://dx.doi.org/10.1293/tox.2017-0035
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author Kuroda, Hiroyuki
Kinomoto, Toshiko
Ogawa, Shuji
Kawabe, Mayumi
Suguro, Mayuko
Naraoka, Hitoshi
Takamatsu, Kazuhiko
Oishi, Yuji
author_facet Kuroda, Hiroyuki
Kinomoto, Toshiko
Ogawa, Shuji
Kawabe, Mayumi
Suguro, Mayuko
Naraoka, Hitoshi
Takamatsu, Kazuhiko
Oishi, Yuji
author_sort Kuroda, Hiroyuki
collection PubMed
description Although acotiamide hydrochloride hydrate (acotiamide-HH) has not been reported to have genotoxic findings in any of the genotoxicity studies or treatment-related toxicological findings in reproductive and developmental studies, suspicious uterine tumorigenesis was observed in the results of a long-term rat carcinogenicity study. To clarify the uterine tumorigenesis of acotiamide-HH, we performed a 2-stage uterine carcinogenicity model in the transgenic rasH2 mouse initiated by N-Ethyl-N-nitrosourea (ENU). This model facilitated the short-term detection of uterine carcinogenic potential, and it appears to be a very useful testing method for assessing the safety of chemicals that may affect uterine tumorigenesis. However, there have not been many reports on this model, and accumulation of case studies using this model is recommended to support its usability. In this study, we performed this carcinogenesis model to not only confirm uterine tumorigenesis of acotiamide-HH but also to confirm the reliability of the model. The results of this study revealed that the endometrial adenocarcinoma found in the long-term rat carcinogenicity study possibly arose spontaneously. Also, we confirmed early induction of a uterine tumor as in previous reports and confirmed that 26 weeks is the appropriate treatment period for this rasH2 mouse model according to time-course observations of uterine tumor development.
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spelling pubmed-58201012018-02-23 Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model Kuroda, Hiroyuki Kinomoto, Toshiko Ogawa, Shuji Kawabe, Mayumi Suguro, Mayuko Naraoka, Hitoshi Takamatsu, Kazuhiko Oishi, Yuji J Toxicol Pathol Original Article Although acotiamide hydrochloride hydrate (acotiamide-HH) has not been reported to have genotoxic findings in any of the genotoxicity studies or treatment-related toxicological findings in reproductive and developmental studies, suspicious uterine tumorigenesis was observed in the results of a long-term rat carcinogenicity study. To clarify the uterine tumorigenesis of acotiamide-HH, we performed a 2-stage uterine carcinogenicity model in the transgenic rasH2 mouse initiated by N-Ethyl-N-nitrosourea (ENU). This model facilitated the short-term detection of uterine carcinogenic potential, and it appears to be a very useful testing method for assessing the safety of chemicals that may affect uterine tumorigenesis. However, there have not been many reports on this model, and accumulation of case studies using this model is recommended to support its usability. In this study, we performed this carcinogenesis model to not only confirm uterine tumorigenesis of acotiamide-HH but also to confirm the reliability of the model. The results of this study revealed that the endometrial adenocarcinoma found in the long-term rat carcinogenicity study possibly arose spontaneously. Also, we confirmed early induction of a uterine tumor as in previous reports and confirmed that 26 weeks is the appropriate treatment period for this rasH2 mouse model according to time-course observations of uterine tumor development. Japanese Society of Toxicologic Pathology 2017-09-21 2018-01 /pmc/articles/PMC5820101/ /pubmed/29479138 http://dx.doi.org/10.1293/tox.2017-0035 Text en ©2018 The Japanese Society of Toxicologic Pathology This is an open-access article distributed under the terms of the Creative Commons Attribution Non-Commercial No Derivatives (by-nc-nd) License. (CC-BY-NC-ND 4.0: https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Article
Kuroda, Hiroyuki
Kinomoto, Toshiko
Ogawa, Shuji
Kawabe, Mayumi
Suguro, Mayuko
Naraoka, Hitoshi
Takamatsu, Kazuhiko
Oishi, Yuji
Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title_full Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title_fullStr Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title_full_unstemmed Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title_short Progression process and safety assessment adaptation of endometrial lesions in ENU-induced 2-stage uterine carcinogenicity in a Tg-rasH2 mouse model
title_sort progression process and safety assessment adaptation of endometrial lesions in enu-induced 2-stage uterine carcinogenicity in a tg-rash2 mouse model
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5820101/
https://www.ncbi.nlm.nih.gov/pubmed/29479138
http://dx.doi.org/10.1293/tox.2017-0035
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