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Flufenamic acid prevents behavioral manifestations of salicylate-induced tinnitus in the rat
Authors:Ramazan Bal  Yasemin Ustundag  Funda Bulut  Caner Feyzi Demir  Ali Bal
Affiliation:1.Department of Physiology, Faculty of Medicine, Gaziantep University, Gaziantep, Turkey;2.Department of Anatomy, Faculty of Veterinary, Firat University, Elazig, Turkey;3.Department of Medical Biology, Faculty of Medicine, Kirikkale University, Kirikkale, Turkey;4.Department of Neurology, Faculty of Medicine, Firat University, Elazig, Turkey;5.Department of Plastic-Reconstructive and Esthetic Surgery, Faculty of Medicine, Firat University, Elazig, Turkey
Abstract:

Introduction

Tinnitus is defined as a phantom auditory sensation, the perception of sound in the absence of external acoustic stimulation. Given that flufenamic acid (FFA) blocks TRPM2 cation channels, resulting in reduced neuronal excitability, we aimed to investigate whether FFA suppresses the behavioral manifestation of sodium salicylate (SSA)-induced tinnitus in rats.

Material and methods

Tinnitus was evaluated using a conditioned lick suppression model of behavioral testing. Thirty-one Wistar rats, randomly divided into four treatment groups, were trained and tested in the behavioral experiment: (1) control group: DMSO + saline (n = 6), (2) SSA group: DMSO + SSA (n = 6), (3) FFA group: FFA (66 mg/kg bw) + saline (n = 9), (4) FFA + SSA group: FFA (66 mg/kg bw) + SSA (400 mg/kg bw) (n = 10). Localization of TRPM2 to the plasma membrane of cochlear nucleus neurons was demonstrated by confocal microscopy.

Results

Pavlovian training resulted in strong suppression of licking, having a mean value of 0.05 ±0.03 on extinction day 1, which is below the suppression training criterion level of 0.20 in control tinnitus animals. The suppression rate for rats having both FFA (66 mg/kg bw) and SSA (400 mg/kg bw) injections was significantly lower than that for the rats having SSA injections (p < 0.01).

Conclusions

We suggest that SSA-induced tinnitus could possibly be prevented by administration of a TRPM2 ion channel antagonist, FFA at 66 mg/kg bw.
Keywords:tinnitus   salicylate   flufenamic acid   TRPM2   experimental   rat
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