Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole

Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole

Sigma-1 receptor (chaperone Sigma1R) is an intracellular protein with chaperone functions, which is expressed in various organs, including the brain. Sigma1R participates in the regulation of physiological mechanisms of anxiety (Su, T. P. et al., 2016) and reactions to emotional stress (Hayashi, T.,...

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Main Authors: Mikhail V. Voronin, Yulia V. Vakhitova, Inna P. Tsypysheva, Dmitry O. Tsypyshev, Inna V. Rybina, Rustam D. Kurbanov, Elena V. Abramova, Sergei B. Seredenin
Format: Article
Language:English
Published: MDPI AG 2021-05-01
Series:International Journal of Molecular Sciences
Subjects:
chaperone Sigma1R
fabomotizole
anxiolytic
elevated plus maze
(+)-pentazocine
NE-100
Online Access:https://www.mdpi.com/1422-0067/22/11/5455
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spelling doaj-88074c245d414c42a2776291d62472082021-06-01T00:46:36ZengMDPI AGInternational Journal of Molecular Sciences1661-65961422-00672021-05-01225455545510.3390/ijms22115455Involvement of Chaperone Sigma1R in the Anxiolytic Effect of FabomotizoleMikhail V. Voronin0Yulia V. Vakhitova1Inna P. Tsypysheva2Dmitry O. Tsypyshev3Inna V. Rybina4Rustam D. Kurbanov5Elena V. Abramova6Sergei B. Seredenin7Department of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaDepartment of Pharmacogenetics, Federal State Budgetary Institution “Research Zakusov Institute of Pharmacology”, Baltiyskaya Street 8, 125315 Moscow, RussiaSigma-1 receptor (chaperone Sigma1R) is an intracellular protein with chaperone functions, which is expressed in various organs, including the brain. Sigma1R participates in the regulation of physiological mechanisms of anxiety (Su, T. P. et al., 2016) and reactions to emotional stress (Hayashi, T., 2015). In 2006, fabomotizole (ethoxy-2-[2-(morpholino)-ethylthio]benzimidazole dihydrochloride) was registered in Russia as an anxiolytic (Seredenin S. and Voronin M., 2009). The molecular targets of fabomotizole are Sigma1R, NRH: quinone reductase 2 (NQO2), and monoamine oxidase A (MAO-A) (Seredenin S. and Voronin M., 2009). The current study aimed to clarify the dependence of fabomotizole anxiolytic action on its interaction with Sigma1R and perform a docking analysis of fabomotizole interaction with Sigma1R. An elevated plus maze (EPM) test revealed that the anxiolytic-like effect of fabomotizole (2.5 mg/kg i.p.) administered to male BALB/c mice 30 min prior EPM exposition was blocked by Sigma1R antagonists BD-1047 (1.0 mg/kg i.p.) and NE-100 (1.0 mg/kg i.p.) pretreatment. Results of initial in silico study showed that fabomotizole locates in the active center of Sigma1R, reproducing the interactions with the site’s amino acids common for established Sigma1R ligands, with the ΔG<sub>bind</sub> value closer to that of agonist (+)-pentazocine in the 6DK1 binding site.https://www.mdpi.com/1422-0067/22/11/5455chaperone Sigma1Rfabomotizoleanxiolyticelevated plus maze(+)-pentazocineNE-100
collection DOAJ
language English
format Article
sources DOAJ
author Mikhail V. Voronin
Yulia V. Vakhitova
Inna P. Tsypysheva
Dmitry O. Tsypyshev
Inna V. Rybina
Rustam D. Kurbanov
Elena V. Abramova
Sergei B. Seredenin
spellingShingle Mikhail V. Voronin
Yulia V. Vakhitova
Inna P. Tsypysheva
Dmitry O. Tsypyshev
Inna V. Rybina
Rustam D. Kurbanov
Elena V. Abramova
Sergei B. Seredenin
Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
International Journal of Molecular Sciences
chaperone Sigma1R
fabomotizole
anxiolytic
elevated plus maze
(+)-pentazocine
NE-100
author_facet Mikhail V. Voronin
Yulia V. Vakhitova
Inna P. Tsypysheva
Dmitry O. Tsypyshev
Inna V. Rybina
Rustam D. Kurbanov
Elena V. Abramova
Sergei B. Seredenin
author_sort Mikhail V. Voronin
title Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
title_short Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
title_full Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
title_fullStr Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
title_full_unstemmed Involvement of Chaperone Sigma1R in the Anxiolytic Effect of Fabomotizole
title_sort involvement of chaperone sigma1r in the anxiolytic effect of fabomotizole
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1661-6596
1422-0067
publishDate 2021-05-01
description Sigma-1 receptor (chaperone Sigma1R) is an intracellular protein with chaperone functions, which is expressed in various organs, including the brain. Sigma1R participates in the regulation of physiological mechanisms of anxiety (Su, T. P. et al., 2016) and reactions to emotional stress (Hayashi, T., 2015). In 2006, fabomotizole (ethoxy-2-[2-(morpholino)-ethylthio]benzimidazole dihydrochloride) was registered in Russia as an anxiolytic (Seredenin S. and Voronin M., 2009). The molecular targets of fabomotizole are Sigma1R, NRH: quinone reductase 2 (NQO2), and monoamine oxidase A (MAO-A) (Seredenin S. and Voronin M., 2009). The current study aimed to clarify the dependence of fabomotizole anxiolytic action on its interaction with Sigma1R and perform a docking analysis of fabomotizole interaction with Sigma1R. An elevated plus maze (EPM) test revealed that the anxiolytic-like effect of fabomotizole (2.5 mg/kg i.p.) administered to male BALB/c mice 30 min prior EPM exposition was blocked by Sigma1R antagonists BD-1047 (1.0 mg/kg i.p.) and NE-100 (1.0 mg/kg i.p.) pretreatment. Results of initial in silico study showed that fabomotizole locates in the active center of Sigma1R, reproducing the interactions with the site’s amino acids common for established Sigma1R ligands, with the ΔG<sub>bind</sub> value closer to that of agonist (+)-pentazocine in the 6DK1 binding site.
topic chaperone Sigma1R
fabomotizole
anxiolytic
elevated plus maze
(+)-pentazocine
NE-100
url https://www.mdpi.com/1422-0067/22/11/5455
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