Polypodium leucotomos targets multiple aspects of oral carcinogenesis and it is a potential antitumor phytotherapy against tongue cancer growth

Polypodium leucotomos targets multiple aspects of oral carcinogenesis and it is a potential antitumor phytotherapy against tongue cancer growth

http://urn.fi/urn:nbn:fi-fe2023070587153

Teksti

Lacerda, P. A. (Pammela A.) ; Oenning, L. C. (Luan C.) ; Bellato, G. C. (Guilherme Cuoghi) ; Lopes-Santos, L. (Lucilene) ; Antunes, N. d. (Natalícia de Jesus) ; Mariz, B. A. (Bruno Augusto Linhares Almeida) ; Teixeira, G. (Gabriela) ; Vasconcelos, R. (Rafael) ; Simões, G. F. (Gustavo Ferreira) ; de Souza, I. A. (Ivani Aparecida) ; Pinto, C. A. (Clóvis Antônio Lopes) ; Salo, T. (Tuula) ; Coletta, R. D. (Ricardo D.) ; Augusto, T. M. (Taize M.) ; de Oliveira, C. E. (Carine Ervolino) ; Cervigne, N. K. (Nilva K.)

Frontiers Media

Abstract

Introduction: Oral cancer refers to malignant tumors, of which 90% are squamous cell carcinomas (OSCCs). These malignancies exhibit rapid progression, poor prognosis, and often mutilating therapeutical approaches. The determination of a prophylactic and/or therapeutic antitumor role of the polyphenolic extract Polypodium leucotomos(PL) would be relevant in developing new tools for prevention and treatment.

Methods: We aimed to determine the antitumor effect of PL by treating OSCC cell lines with PL metabolites and evaluating its action during OSCC progression in vivo.

Results: PL treatment successfully impaired cell cycling and proliferation, migration, and invasion, enhanced apoptosis, and modulated macrophage polarization associated with the tumoral immune-inflammatory response of tongue cancer cell lines (TSCC). PL treatment significantly decreased the expression of MMP1 (p < 0.01) and MMP2 (p < 0.001), and increased the expression of TIMP1 (p < 0.001) and TIMP2 (p < 0.0001) in these cells. The mesenchymal-epithelial transition phenotype was promoted in cells treated with PL, through upregulation of E-CAD (p < 0.001) and reduction of N-CAD (p < 0.05). PL restrained OSCC progression in vivo by inhibiting tumor volume growth and decreasing the number of severe dysplasia lesions and squamous cell carcinomas. Ki-67 was significantly higher expressed in tongue tissues of animals not treated with PL(p < 0.05), and a notable reduction in Bcl2 (p < 0.05) and Pcna (p < 0.05) cell proliferation-associated genes was found in dysplastic lesions and TSCCs of PL-treated mice. Finally, N-cad(Cdh2), Vim, and Twist were significantly reduced in tongue tissues treated with PL.

Conclusions: PL significantly decreased OSCC carcinogenic processes in vitro and inhibited tumor progression in vivo. PL also appears to contribute to the modulation of immune-inflammatory oral tumor-associated responses. Taken together, these results suggest that PL plays an important antitumor role in processes associated with oral carcinogenesis and may be a potential phytotherapeutic target for the prevention and/or adjuvant treatment of TSCCs.

Tallennettuna:

Ulkoasu

application/pdf

Kieli

englanti

Asiasanat

EMT-epithelial to mesenchymal transformation