Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells

Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells

A functional understanding of the relationship between glucocorticoids and neuronal apoptosis induced by the production of reactive oxygen species (ROS) may lead to a novel strategy for the treatment or prevention of depression. Previous reports suggest that butein, a type of flavonoids, may be a po...

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Main Authors: Masanori Ohmoto, Yukina Shibuya, Shihori Taniguchi, Tomoki Nakade, Masaaki Nomura, Yuri Ikeda-Matsuo, Tohru Daikoku
Format: Article
Language:English
Published: Elsevier 2020-06-01
Series:IBRO Reports
Subjects:
Butein
Corticosterone
Apoptosis
Neurite outgrowth
ROS
Neuro2A cells
Online Access:http://www.sciencedirect.com/science/article/pii/S2451830120300066
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spelling doaj-fecde1ac4bf54c2da1257939e797d7a52020-11-25T02:47:08ZengElsevierIBRO Reports2451-83012020-06-0188290Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cellsMasanori Ohmoto0Yukina Shibuya1Shihori Taniguchi2Tomoki Nakade3Masaaki Nomura4Yuri Ikeda-Matsuo5Tohru Daikoku6Department of Pharmacy Practice and Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, Japan; Corresponding author at: Department of Pharmacy Practice and Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, Ho-3 Kanagawa-machi, Kanazawa, 920-1181, Japan.Department of Pharmacy Practice and Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanDepartment of Pharmacy Practice and Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanDepartment of Pharmacy Practice and Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanDepartment of Clinical Pharmacy, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanDepartment of Clinical Pharmacy, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanDepartment of Pharmaceutical Life Sciences, Faculty of Pharmaceutical Sciences, Hokuriku University, JapanA functional understanding of the relationship between glucocorticoids and neuronal apoptosis induced by the production of reactive oxygen species (ROS) may lead to a novel strategy for the treatment or prevention of depression. Previous reports suggest that butein, a type of flavonoids, may be a potent candidate against depression-related neuronal cell apoptosis caused by oxidative stress; however, the protective effects of butein on damaged corticosterone (CORT)-treated neuronal cells has not been elucidated. In the present study, we examined the protective effect of butein on CORT-induced cytotoxicity and neurite growth during cell differentiation of mouse neuroblastoma Neuro2A (N2A) cells. Moreover, the effect on cultured cells by high concentrations of butein was confirmed. Our results demonstrate that CORT treatment significantly decreases cell viability and induces cell death. CORT was suggested to induce apoptosis via mitochondrial dysfunction and caspase-3 activation; this apoptosis may be attributed to DNA damage by ROS generation, found in this study to be significantly inhibited by pretreatment with butein. We found that CORT produced significant growth suppression of retinoic acid-induced neurite outgrowth in N2A cells; however, butein significantly increased neurite length and induced dose-dependent apoptotic cytotoxicity in N2A cells. This study suggests that low concentration of butein can prevent CORT-induced cytotoxicity in N2A cells, and provides preliminary results supporting some of the beneficial roles of butein in neuroprotection.http://www.sciencedirect.com/science/article/pii/S2451830120300066ButeinCorticosteroneApoptosisNeurite outgrowthROSNeuro2A cells
collection DOAJ
language English
format Article
sources DOAJ
author Masanori Ohmoto
Yukina Shibuya
Shihori Taniguchi
Tomoki Nakade
Masaaki Nomura
Yuri Ikeda-Matsuo
Tohru Daikoku
spellingShingle Masanori Ohmoto
Yukina Shibuya
Shihori Taniguchi
Tomoki Nakade
Masaaki Nomura
Yuri Ikeda-Matsuo
Tohru Daikoku
Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
IBRO Reports
Butein
Corticosterone
Apoptosis
Neurite outgrowth
ROS
Neuro2A cells
author_facet Masanori Ohmoto
Yukina Shibuya
Shihori Taniguchi
Tomoki Nakade
Masaaki Nomura
Yuri Ikeda-Matsuo
Tohru Daikoku
author_sort Masanori Ohmoto
title Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
title_short Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
title_full Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
title_fullStr Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
title_full_unstemmed Protective effects of butein on corticosterone-induced cytotoxicity in Neuro2A cells
title_sort protective effects of butein on corticosterone-induced cytotoxicity in neuro2a cells
publisher Elsevier
series IBRO Reports
issn 2451-8301
publishDate 2020-06-01
description A functional understanding of the relationship between glucocorticoids and neuronal apoptosis induced by the production of reactive oxygen species (ROS) may lead to a novel strategy for the treatment or prevention of depression. Previous reports suggest that butein, a type of flavonoids, may be a potent candidate against depression-related neuronal cell apoptosis caused by oxidative stress; however, the protective effects of butein on damaged corticosterone (CORT)-treated neuronal cells has not been elucidated. In the present study, we examined the protective effect of butein on CORT-induced cytotoxicity and neurite growth during cell differentiation of mouse neuroblastoma Neuro2A (N2A) cells. Moreover, the effect on cultured cells by high concentrations of butein was confirmed. Our results demonstrate that CORT treatment significantly decreases cell viability and induces cell death. CORT was suggested to induce apoptosis via mitochondrial dysfunction and caspase-3 activation; this apoptosis may be attributed to DNA damage by ROS generation, found in this study to be significantly inhibited by pretreatment with butein. We found that CORT produced significant growth suppression of retinoic acid-induced neurite outgrowth in N2A cells; however, butein significantly increased neurite length and induced dose-dependent apoptotic cytotoxicity in N2A cells. This study suggests that low concentration of butein can prevent CORT-induced cytotoxicity in N2A cells, and provides preliminary results supporting some of the beneficial roles of butein in neuroprotection.
topic Butein
Corticosterone
Apoptosis
Neurite outgrowth
ROS
Neuro2A cells
url http://www.sciencedirect.com/science/article/pii/S2451830120300066
work_keys_str_mv AT masanoriohmoto protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT yukinashibuya protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT shihoritaniguchi protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT tomokinakade protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT masaakinomura protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT yuriikedamatsuo protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
AT tohrudaikoku protectiveeffectsofbuteinoncorticosteroneinducedcytotoxicityinneuro2acells
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