γ-Terpinene complexed with β-cyclodextrin attenuates spinal neuroactivity in animals with cancer pain by Ca2+ channel block

Author:

Pina Lícia T S1,Rabelo Thallita K2,Trindade Gabriela G G1,Almeida Iggo K S1,Oliveira Marlange A3,dos Santos Priscila L3,Souza Diego Santos45,de Menezes-Filho José E R6,de Vasconcelos Carla Maria Lins3ORCID,Santos Sandra L3,Scotti Luciana7,Scotti Marcus T7,Araújo Adriano A S1,Quintans Jullyana S S3,Quintans Lucindo J3,Guimarães Adriana G1ORCID

Affiliation:

1. Department of Pharmacy, Federal University of Sergipe , São Cristóvão, Sergipe , Brazil

2. Sunnybrook Research Institute. Harquail Centre for Neuromodulation , Canada

3. Department of Physiology, Federal University of Sergipe , São Cristóvão, Sergipe , Brazil

4. Department of Biophysics and Immunology, Federal University of Minas Gerais , Brazil

5. Department of Biophysics, Federal University of São Paulo , São Paulo , Brazil

6. Department of Biochemistry and Immunology, Federal University of Minas Gerais , Brazil

7. Federal University of Paraiba , João Pessoa, Paraíba , Brazil

Abstract

Abstract Objectives Considering that γ-terpinene (γ-TPN) is a monoterpene found in Cannabis oil, with high lipophilicity and limited pharmacokinetics, our objective was to evaluate whether its complexation in β-cyclodextrin (γ-TPN/β-CD) could improve its physicochemical properties and action on cancer pain, as well as verify the mechanisms of action involved. Methods The γ-TPN/β-CD was prepared and submitted to physicochemical characterization. Animals with sarcoma 180 were treated (vehicle, γ-TPN 50 mg/kg, γ-TPN/β-CD 5 mg/kg or morphine) and assessed for hyperalgesia, TNF-α and IL-1β levels, iNOS and c-Fos activity. The effects of γ-TPN on calcium channels were studied by patch-clamp and molecular docking. Results β-CD improved the physicochemical properties and prolonged the anti-hyperalgesic effect of γ-TPN. This compound also reduced the levels of IL-1β, TNF-α and iNOS in the tumour, and c-Fos protein in the spinal cord. In addition, it reduced Ca2+ current, presenting favourable chemical interactions with different voltage-dependent calcium channels. Conclusion These results indicate that the complexation of γ-TPN into β-CD increases its stability and time effect, reducing spinal neuroactivity and inflammation by blocking calcium channels.

Publisher

Oxford University Press (OUP)

Subject

Pharmaceutical Science,Pharmacology

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