Afobazole metabolite M-11 inhibits quinone reductase 2

I. A. Kadnikov; M. V. Voronin; S. B. Seredenin

doi:10.24411/2587-7836-2018-10020.

Фармакокинетика и Фармакодинамика (Oct 2019)

Afobazole metabolite M-11 inhibits quinone reductase 2

I. A. Kadnikov,
M. V. Voronin,
S. B. Seredenin

Affiliations

I. A. Kadnikov: FSBI «Zakusov institute of Pharmacology»
M. V. Voronin: FSBI «Zakusov institute of Pharmacology»
S. B. Seredenin: FSBI «Zakusov institute of Pharmacology»

DOI: https://doi.org/10.24411/2587-7836-2018-10020.
Journal volume & issue: Vol. 0, no. 3
pp. 27 – 30

Abstract

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Resume. Objective. Inhibition of quinone reductase 2 (NQO2) is a perspective target to achieve neuroprotective effect. Anxiolytic drug afobazole (5-Ethoxy-2-[2-(morpholino)-ethylthio]benzimidazole dihidrochloride) and its main metabolite M-11 (2-[2-(3-oxomorpholin-4-il)-ethylthio]-5-ethoxybenzimidazole hydrochloride) can interact with melatonin dependent regulatory site of NQO2. Previously we have figured that afobazole inhibits NQO2. However, the role of interaction between M-11 and NQO2 is unclear. Aim. To study the effect of M-11 on activity of NQO2. Methods. The influence of M-11 on activity of human recombinant NQO2 (hNQO2) was measured utilizing fluorescent spectroscopy. Results. M-11 inhibits hNQO2 in concentrations of 0.5 and 1.0 mM, decreasing enzymatic reaction velocity on 12 and 24 % respectively. In same concentrations, M-11 is inferior to afobazole. Conclusion. Compound M-11 inhibits NQO2 and can be used to study pharmacological effects of afobazole caused by interaction with regulatory site of enzyme.

Published in Фармакокинетика и Фармакодинамика

ISSN: 2587-7836 (Print); 2686-8830 (Online)
Publisher: LLC “Publisher OKI”
Country of publisher: Russian Federation
LCC subjects: Medicine: Pharmacy and materia medica
Website: https://www.pharmacokinetica.ru/

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