Three (―)-cytisine derivatives and 1-hydroxyquinopimaric acid as acetylcholinesterase inhibitors

J. Daniel García-García; E. Patricia Segura-Ceniceros; Radik A. Zaynullin; Raikhana V. Kunakova; Guzel F. Vafina; Inna P. Tsypysheva; Alejandra I. Vargas-Segura; Anna Ilyina

Toxicology Reports (Jan 2019)

Three (―)-cytisine derivatives and 1-hydroxyquinopimaric acid as acetylcholinesterase inhibitors

J. Daniel García-García,
E. Patricia Segura-Ceniceros,
Radik A. Zaynullin,
Raikhana V. Kunakova,
Guzel F. Vafina,
Inna P. Tsypysheva,
Alejandra I. Vargas-Segura,
Anna Ilyina

Affiliations

J. Daniel García-García: Nanobioscience Group, Chemistry School, Autonomous University of Coahuila, Blvd. V. Carranza e Ing. J. Cardenas V., Saltillo, Coahuila, CP. 25280, Mexico
E. Patricia Segura-Ceniceros: Nanobioscience Group, Chemistry School, Autonomous University of Coahuila, Blvd. V. Carranza e Ing. J. Cardenas V., Saltillo, Coahuila, CP. 25280, Mexico
Radik A. Zaynullin: Ufa State Petroleum Technological University, 1 Cosmonauts St., Ufa, Bashkortostan, 450062, Russia
Raikhana V. Kunakova: Ufa State Petroleum Technological University, 1 Cosmonauts St., Ufa, Bashkortostan, 450062, Russia
Guzel F. Vafina: Ufa Institute of Chemistry of Russian Academy of Science, Ufa, 71 Prospekt Oktyabrya, Ufa, Bashkortostan, 450054, Russia
Inna P. Tsypysheva: Ufa Institute of Chemistry of Russian Academy of Science, Ufa, 71 Prospekt Oktyabrya, Ufa, Bashkortostan, 450054, Russia
Alejandra I. Vargas-Segura: Nanobioscience Group, Chemistry School, Autonomous University of Coahuila, Blvd. V. Carranza e Ing. J. Cardenas V., Saltillo, Coahuila, CP. 25280, Mexico
Anna Ilyina: Nanobioscience Group, Chemistry School, Autonomous University of Coahuila, Blvd. V. Carranza e Ing. J. Cardenas V., Saltillo, Coahuila, CP. 25280, Mexico; Corresponding author.

Journal volume & issue: Vol. 6
pp. 862 – 868

Abstract

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In vitro acetylcholinesterase (AChE) inhibition was studied using novel derivatives of (―)-cytisine derivatives N-allylcytisine-12-carbamide (A-63), cytisine-12-carbamide (A-36), N-1-adamantylcytisine-12-thiocarbamide (U-12), and 1-hydroxyquinopimaric acid (U-201). Inhibition of acetylcholinesterase with compound A-63 was described as mixed inhibition. Substances (A-36) and (U-201) acted as competitive inhibitors with Ki equal to 6.71 mM and 3.89 mM, respectively, while (U-12) behaved as an uncompetitive inhibitor with Ki at 0.07 mM. The IC50 values were estimated at 1.47, 13.73, 3.39, and 7.81 mM, respectively. According to toxicity assessment, compound A-63 was non-toxic; it did not affect A. salina viability at a concentration less than 1000 ppm, while at 1000 ppm, only 3% mortality was observed. Mortality of A. salina was less than 50% in the same concentration range for the other three compounds that allow classifying them as moderately toxic. Although tested compounds have the characteristics of weak inhibitors, they could be useful as protectors against potent organophosphates. The present research may be fundamental to the design of new substances for acetylcholinesterase inhibition. Keywords: Acetylcholinesterase inhibition, (-)-Cytisine derivatives, 1-Hydroxyquinopimaric acid, Toxicity on Artemia salina model

Published in Toxicology Reports

ISSN: 2214-7500 (Online)
Publisher: Elsevier
Country of publisher: Ireland
LCC subjects: Medicine: Public aspects of medicine: Toxicology. Poisons
Website: http://www.journals.elsevier.com/toxicology-reports/

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