Anticonvulsant effects of desvenlafaxine on modulating brain monoamine and oxidative stress in mice

Alharbi, Khalid Saad

doi:10.1590/1519-6984.246194

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Brazilian Journal of Biology

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Original Article • Braz. J. Biol. 83 • 2023 • https://doi.org/10.1590/1519-6984.246194 copy

Anticonvulsant effects of desvenlafaxine on modulating brain monoamine and oxidative stress in mice

Efeitos anticonvulsivantes da desvenlafaxina na modulação da monoamina cerebral e do estresse oxidativo em camundongos

Authorship SCIMAGO INSTITUTIONS RANKINGS

Abstract

Desvenlafaxine succinate (DVS) inhibits serotonin reuptake selectively and is approved for major depressive disorders. This research investigated influence of DVS on modulating brain monoamine and oxidative stress in mice. The antiepileptic potential of DVS (10, 20, or 30 mg/kg/i.p.) in pentylenetetrazole (PTZ; 85 mg/kg) with i.p. route of administration, strychnine (STR; 75 mg/kg) with i.p. route, pilocarpine (400 mg/kg) with s.c. route and maximal electroshock MES-induced convulsion in mouse models. The activities of oxidative stress, i.e. superoxide dismutase (SOD), glutathione (GSH) and lipid peroxidation (LPO) as well as gamma-aminobutyric acid (GABA) in the brains of PTZ-induced convulsive mice. Treatment with DVS increased the latency to develop siezures and declined mortalities in rodents against PTZ, STR and pilocarpine-induced convulsions. Results of MES-leaded siezures revealed that DVS reduced tonic hind limb extension duration and mortalities significantly. Brain, SOD, GSH and GABA level were significantly (P<0.01) increased and LPO reduced significantly (P<0.01) after DVS treatment. Furthermore, the DVS did not show any motor coordination signs in the rotarod test. We demonstrated that the role of DVS in convulsion genesis in mice under control condition and attenuate the PTZ-induced oxidative damage.

Keywords:
anticonvulsant effect; Desvenlafaxine; oxidative stress; Pentylenetetrazol

Group	Dose (mg/kg, i.p.)	Latency for convulsion (sec)	Duration of myoclonic jerks (sec)	% protection against seizures	% protection against mortality
Control	10 ml	118.3 ± 7.5	12.5 ± 1.2	0	0
DVS	10	182.2 ± 8.8	21.5 ± 0.7	58.2	60
	20	244.8 ± 18.7*	25.6 ± 0.9^*	76.8	78
	30	269.7 ± 17.1*	29.8 ± 0.4*	80.3	80

Group	Dose (mg/kg, i.p.)	Latency for convulsion (sec)	Duration of myoclonic jerks (sec)	% protection against seizures	% protection against mortality
Control	10 ml	25.5 ± 3.0	12.50 ± 1.1	0	0
DVS	10	45.5 ± 3.5	18.50 ± 1.3	34.0	35.9
	20	54.5 ± 4.4*	20.49 ± 2.4^*	47.5	46.0
	30	80.6 ± 5.6*	25.83 ± 2.6*	55.9	58.7

Group	Dose (mg/kg, i.p.)	Latency for convulsion (sec)	Duration of myoclonic jerks (sec)	% protection against seizures	% protection against mortality
Control	10 ml	410.3 ± 44.9	15.50 ± 1.2	0	0
DVS	10	716.8 ± 29.6	19.50 ± 0.7	51.2	59.9
	20	844.0 ± 59.5	22.66 ± 0.9*	60.5	68.5
	30	1040.0 ± 45.4*	24.83 ± 0.4*	69.7	71.2

Group	Dose (mg/kg, i.p.)	Duration of hind limb extension (sec)	% protection against seizures	% protection against mortality
Control	10 ml	10.3 ± 1.1	0	0
DVS	10	5.8 ± 0.4	50.0	63.1
	20	3.0 ± 0.5*	67.5	83.3
	30	0.8 ± 0.3*	91.3	98.6

Group	Dose (mg/kg, i.p.)	GABA (ng/g of brain tissue)
Control	10 ml	17.5 ± 1.0
DVS	10	22.4 ± 0.5^*
	20	31.5 ± 0.5^**
	30	48.3 ± 0.5**

Group	Dose (mg/kg, i.p.)	MDA (nmol/g of brain tissue)	SOD (U/mg of protein)	GSH (μg/mg of protein)
Control	10 ml	2.3 ± 1.0	3.40 ± 0.4	0.80 ± 0.05
DVS	10	1.7 ± 0.5^*	7.80 ± 0.5*	2.15 ± 0.3*
	20	1.5 ± 0.5^**	10.20 ± 0.7**	2.68 ± 0.3**
	30	1.2 ± 0.5**	10.90 ± 0.7**	2.78 ± 0.2**

Instituto Internacional de Ecologia R. Bento Carlos, 750, 13560-660 São Carlos SP - Brasil, Tel. e Fax: (55 16) 3362-5400 - São Carlos - SP - Brazil
E-mail: bjb@bjb.com.br

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[1] *e-mail: kssalharbi@ju.edu.sa