Antinociceptive Activity of : and Studies

Overview

Journal Front Pharmacol

Date 2017 Jun 8

PMID 28588488

Citations 5

Authors

Rosa H M Silva

Nathalia de Fatima M Lima

Alberto J O Lopes

Cleydlenne C Vasconcelos

Jose W C de Mesquita

Ludmilla S S de Mesquita

Fernando C V M Lima

Maria N de S Ribeiro

Ricardo M Ramos

Maria do Socorro de S Cartagenes

Joao B S Garcia

Affiliations

Soon will be listed here.

Abstract

(L.) G. Mey. known vassourinha has antibacterial, antimalarial, hepatoprotective, antioxidative, analgesic, and anti-inflammatory, however, its antinociceptive action requires further studies. Aim of the study evaluated the antinociceptive activity of hydroalcoholic extract (EHBv) and ethyl acetate fraction (FAc) by and studies. assessment included the paw edema test, writhing test, formalin test and tail flick test. Wistar rats and Swiss mice were divided into 6 groups and given the following treatments oral: 0.9% NaCl control group (CTRL), 10 mg/kg memantine (MEM), 10 mg/kg indomethacin (INDO), 500 mg/kg EHBv (EHBv 500), 25 mg/kg FAc (FAc 25) and 50 mg/kg FAc (FAc 50). EHBv, FAc 25 and 50 treatments exhibited anti-edematous and peripheral antinociceptive effects. For assessment, compounds identified in FAc were subjected to molecular docking with COX-2, GluN1a and GluN2B. Ursolic acid (UA) was the compound with best affinity parameters (binding energy and inhibition constant) for COX-2, GluN1a, GluN2B, and was selected for further analysis with molecular dynamics (MD) simulations. In MD simulations, UA exhibited highly frequent interactions with residues Arg120 and Glu524 in the COX-2 active site and NMDA, whereby it might prevent COX-2 and NMDA receptor activation. Treatment with UA 10 mg/Kg showed peripheral and central antinociceptive effect. The antinociceptive effect of might be predominantly attributed to peripheral actions, including the participation of anti-inflammatory components. Ursolic acid is the main active component and seems to be a promising source of COX-2 inhibitors and NMDA receptor antagonists.

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