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Derivatives of 9-phosphorylated acridine as butyrylcholinesterase inhibitors with antioxidant activity and the ability to inhibit ß-amyloid self-aggregation: potential therapeutic agents for Alzheimer's disease.
Makhaeva, Galina F; Kovaleva, Nadezhda V; Rudakova, Elena V; Boltneva, Natalia P; Lushchekina, Sofya V; Astakhova, Tatiana Yu; Timokhina, Elena N; Serebryakova, Olga G; Shchepochkin, Alexander V; Averkov, Maxim A; Utepova, Irina A; Demina, Nadezhda S; Radchenko, Eugene V; Palyulin, Vladimir A; Fisenko, Vladimir P; Bachurin, Sergey O; Chupakhin, Oleg N; Charushin, Valery N; Richardson, Rudy J.
Affiliation
  • Makhaeva GF; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Kovaleva NV; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Rudakova EV; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Boltneva NP; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Lushchekina SV; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Astakhova TY; Emanuel Institute of Biochemical Physics, Russian Academy of Sciences, Moscow, Russia.
  • Timokhina EN; Emanuel Institute of Biochemical Physics, Russian Academy of Sciences, Moscow, Russia.
  • Serebryakova OG; Emanuel Institute of Biochemical Physics, Russian Academy of Sciences, Moscow, Russia.
  • Shchepochkin AV; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Averkov MA; Institute of Organic Synthesis, Russian Academy of Sciences, Yekaterinburg, Russia.
  • Utepova IA; Department of Organic and Biomolecular Chemistry, Ural Federal University, Yekaterinburg, Russia.
  • Demina NS; Institute of Organic Synthesis, Russian Academy of Sciences, Yekaterinburg, Russia.
  • Radchenko EV; Department of Organic and Biomolecular Chemistry, Ural Federal University, Yekaterinburg, Russia.
  • Palyulin VA; Institute of Organic Synthesis, Russian Academy of Sciences, Yekaterinburg, Russia.
  • Fisenko VP; Department of Organic and Biomolecular Chemistry, Ural Federal University, Yekaterinburg, Russia.
  • Bachurin SO; Institute of Organic Synthesis, Russian Academy of Sciences, Yekaterinburg, Russia.
  • Chupakhin ON; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
  • Charushin VN; Department of Chemistry, Lomonosov Moscow State University, Moscow, Russia.
  • Richardson RJ; Institute of Physiologically Active Compounds at Federal Research Center of Problems of Chemical Physics and Medicinal Chemistry, Russian Academy of Sciences, Chernogolovka, Russia.
Front Pharmacol ; 14: 1219980, 2023.
Article in En | MEDLINE | ID: mdl-37654616
ABSTRACT
We investigated the inhibitory activities of novel 9-phosphoryl-9,10-dihydroacridines and 9-phosphorylacridines against acetylcholinesterase (AChE), butyrylcholinesterase (BChE), and carboxylesterase (CES). We also studied the abilities of the new compounds to interfere with the self-aggregation of ß-amyloid (Aß42) in the thioflavin test as well as their antioxidant activities in the ABTS and FRAP assays. We used molecular docking, molecular dynamics simulations, and quantum-chemical calculations to explain experimental results. All new compounds weakly inhibited AChE and off-target CES. Dihydroacridines with aryl substituents in the phosphoryl moiety inhibited BChE; the most active were the dibenzyloxy derivative 1d and its diphenethyl bioisostere 1e (IC50 = 2.90 ± 0.23 µM and 3.22 ± 0.25 µM, respectively). Only one acridine, 2d, an analog of dihydroacridine, 1d, was an effective BChE inhibitor (IC50 = 6.90 ± 0.55 µM), consistent with docking results. Dihydroacridines inhibited Aß42 self-aggregation; 1d and 1e were the most active (58.9% ± 4.7% and 46.9% ± 4.2%, respectively). All dihydroacridines 1 demonstrated high ABTS•+-scavenging and iron-reducing activities comparable to Trolox, but acridines 2 were almost inactive. Observed features were well explained by quantum-chemical calculations. ADMET parameters calculated for all compounds predicted favorable intestinal absorption, good blood-brain barrier permeability, and low cardiac toxicity. Overall, the best results were obtained for two dihydroacridine derivatives 1d and 1e with dibenzyloxy and diphenethyl substituents in the phosphoryl moiety. These compounds displayed high inhibition of BChE activity and Aß42 self-aggregation, high antioxidant activity, and favorable predicted ADMET profiles. Therefore, we consider 1d and 1e as lead compounds for further in-depth studies as potential anti-AD preparations.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: Front Pharmacol Year: 2023 Document type: Article Affiliation country: RUSSIA
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: Front Pharmacol Year: 2023 Document type: Article Affiliation country: RUSSIA