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Adv Pharm Bull. 2019;9(4): 674-684.
doi: 10.15171/apb.2019.079
PMID: 31857974
PMCID: PMC6912183
Scopus ID: 85075837479
  Abstract View: 1466
  PDF Download: 822

Research Article

Molecular Docking and Preclinical Study of Five-Membered S,S-Palladaheterocycle as Hepatoprotective Agent

Nail Salavatovich Akhmadiev 1 ORCID logo, Albina Midkhatovna Galimova 2, Vnira Rakhimovna Akhmetova 1* ORCID logo, Veronika Radievna Khairullina 3, Rozaliia Akramovna Galimova 2, Eduard Feliksovich Agletdinov 2, Askhat Gabdrahmanovich Ibragimov 1 ORCID logo, Valery Alekseevich Kataev 2

1 Institute of Petrochemistry and Catalysis, Russian Academy of Sciences, 141 Prospekt Oktyabrya, 450075 Ufa, Russia.
2 Bashkir State Medical University, 3 Lenin Str., 450008 Ufa, Russia.
3 Bashkir State University, 32 Zaki Validi Str., 450076 Ufa, Russia.
*Corresponding Author: Email: vnirara@mail.ru

Abstract

Purpose: In order to investigate mechanisms underlying the hepatoprotective action of S,Spalladaheterocycle, inhibition of cytochromes P450 has been modeled by molecular docking of four palladaheterocycle stereoisomers to the active sites of an enzymatic oxidase system. To obtain a deeper insight into biochemical aspects providing a basis for the therapeutic effects of five-membered palladacycles (as mixture of stereoisomers), a number of preclinical trials has been conducted

Methods: 2D and 3D structures of palladaheterocycle stereoisomers were obtained via converting into SDF files by means of software MarvinSketch. Binding of palladaheterocycle at the active sites of cytochromes P450 2E1 and P450 2C9 has been studied by molecular docking using LeadIT 2.3.2. Hepatoprotective activity of palladaheterocycle at 2.5, 25 and 250 mg/kg doses has been studied based on a model of acute intoxication by CCl4 using in vivo methods.

Results: By molecular docking it was identify amino acid fragments responsible for binding with palladacyclic isomers. The tested compound is comparable, in terms of its activity to the hepatoprotective drug SAM according to the in vivo and in vitro experiments such as animal survival data, the efficiency of correction of the cytolytic syndrome, the liver excretory function, carbohydrate, protein and lipid metabolism, and the correction efficiency of the liver antitoxic function (the latter has been determined based on the results of a hexobarbital control experiment).

Conclusion: Taking into account results obtained in vivo, in vitro and in silico, it can be concluded that the five-membered S,S-palladaheterocycle effectively protect the liver against acute damage caused by CCl4 , via activation of catalase and glucuronyltransferase, as well as via inhibition of the oxidative stress enzymes.


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Submitted: 20 Feb 2019
Revision: 05 Jun 2019
Accepted: 06 Jun 2019
ePublished: 08 Jun 2019
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