Document details

The cyclooxigenase-2 Inhibitor parecoxib prevents epidermal dysplasia in HPV16-transgenic mice: efficacy and safety observations

Author(s): Ferreira, Tiago ; Campos, Sandra ; Silva, Mónica G. ; Ribeiro, Rita ; Santos, Susana ; Almeida, José ; Pires, Maria João ; Costa, Rui Miguel G. da ; Marcos, Cláudia Córdova ; Nogueira, António ; Neuparth, Maria João ; Medeiros, Rui ; Bastos, Margarida Maria da Silva Monteiro ; Gaivão, Isabel ; Peixoto, Francisco ; Oliveira, Maria Manuel ; Oliveira, Paula Alexandra

Date: 2019

Persistent ID: http://hdl.handle.net/10400.11/7312

Origin: Repositório Científico do Instituto Politécnico de Castelo Branco

Subject(s): Animals; Anticarcinogenic agents; Cyclooxygenase 2 Inhibitors; Female; Human papillomavirus 16; Isoxazoles; Mice; Mice transgenic; Papillomavirus infections; Skin; Skin neoplasms


Description

Carcinogenesis induced by high-risk human papillomavirus (HPV) involves inflammatory phenomena, partially mediated by cyclooxigenase-2. In pre-clinical models of HPV-induced cancer, cyclooxygenase-2 inhibitors have shown significant efficacy, but also considerable toxicity. This study addresses the chemopreventive effect and hepatic toxicity of a specific cyclooxigensase-2 inhibitor, parecoxib, in HPV16-transgenic mice. Forty-three 20 weeks-old female mice were divided into four groups: I (HPV16-/-, n = 10, parecoxib-treated); II (HPV16-/-n = 11, untreated); III (HPV16+/-, n = 11, parecoxib-treated) and IV (HPV16+/-, n = 11, untreated). Parecoxib (5.0 mg/kg once daily) or vehicle was administered intraperitoneally for 22 consecutive days. Skin lesions were classified histologically. Toxicological endpoints included genotoxic parameters, hepatic oxidative stress, transaminases and histology. Parecoxib completely prevented the onset of epidermal dysplasia in HPV16+/- treated animals (0% versus 64% in HPV16+/- untreated, p = 0.027). Parecoxib decreases lipid peroxidation (LPO) and superoxide dismutase (SOD) activity and increases the GSH:GSSG ratio in HPV16+/- treated animals meaning that oxidative stress is lower. Parecoxib increased genotoxic stress parameters in wild-type and HPV16-transgenic mice, but didn't modify histological or biochemical hepatic parameters. These results indicate that parecoxib has chemopreventive effects against HPV16-induced lesions while maintaining an acceptable toxicological profile in this model.

Document Type Journal article
Language English
Contributor(s) Repositório Científico do Instituto Politécnico de Castelo Branco
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