Anticonvulsant, Anxiolytic and Antidepressant Properties of the β-caryophyllene in Swiss Mice: Involvement of Benzodiazepine-GABAAergic, Serotonergic and Nitrergic Systems

Author:

da Silva Oliveira George L.1ORCID,da Silva José C. Correia L.2,dos Santos C. L da Silva Ana P.3ORCID,Feitosa Chistiane M.4ORCID,de Castro Almeida Fernanda R.5ORCID

Affiliation:

1. Department of Biology, Federal Institute of Mato Grosso, Guaranta do Norte - MT, 78520-000, Guaranta do Norte Campus, Brazil

2. Department of Computer Science, Federal University of Piaui, Teresina, 64049-550, Piaui, Brazil

3. Department of Pharmacy, Federal University of Piaui, 64049-550, Teresina, Brazil

4. Department of Chemistry, University Federal of Piaui, 64049-550, Teresina, Brazil

5. Center for Research on Medicinal Plants, Federal University of Piaui, 64049-550 Teresina, Brazil

Abstract

Background: Central nervous system disorders such as anxiety, depression and epilepsy are characterized by sharing several molecular mechanisms in common and the involvement of the L-arginine/NO pathway in neurobehavioral studies with β-caryophyllene is still little discussed. Objectives: One of the objectives of the present study was to demonstrate the anxiolytic behavioral effect of β-caryophyllene (β-CBP) in female Swiss mice, as well as to investigate the molecular mechanisms underlying the results obtained. Methods: This study evaluated the neurobehavioral effects of β-CBP using the open field test, rota-rod test, elevated plus maze test, novelty suppressed feeding test, tail suspension test and forced swim test, as well as pilocarpine, pentylenetetrazole and isoniazid-induced epileptic seizure models. Results:: The results demonstrated that the neuropharmacological activities of β-CBP may involve benzodiazepine/GABAergic receptors, since the pre-treatment of β-CBP (200 mg/kg) associated with flumazenil (5 mg/kg, benzodiazepine receptor antagonist) and bicuculline (1 mg/kg, selective GABAA receptor antagonist) reestablished the anxiety parameters in the elevated plus-maze test, as well as the results of reduced latency to consume food in the novelty suppressed feeding test. In addition to benzodiazepine/GABAergic receptors, the neuropharmacological properties of β-CBP may be related to inhibition of nitric oxide synthesis, since pre-treatment with L-arginine (500- 750 mg/kg) reversed significantly the anxiolytic, antidepressant and anticonvulsant activities of β-CBP. Conclusion: The results obtained provide additional support in understanding the neuromolecular mechanisms underlying the anxiolytic, antidepressant and anticonvulsive properties of β-CBP in female Swiss mice.

Publisher

Bentham Science Publishers Ltd.

Subject

General Health Professions

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