Effects of artemisinin and cisplatin on the malignant progression of oral leukoplakia. In vitro and in vivo study

青蒿素和顺铂对口腔白斑恶性进展的影响。体外和体内研究

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作者:Mateus José Dutra, Isabella Souza Malta, Maria Leticia de Almeida Lança, Luana Marotta Reis de Vasconcellos, Daniela Adorno-Farias, José Antonio Jara, Estela Kaminagakura

Conclusion

Expression of proteins related to ICD and apoptosis did not increase with treatments, and CSP was shown to reduce immunogenic pathways in SCC-180, while reducing cell migration. ART did not prevent the malignant progression of OL in vivo; CSP did despite significant adverse effects.

Methods

Normal keratinocytes (HaCat), Dysplastic oral cells (DOK), and oral squamous cell carcinoma (SCC-180) cell lines were treated with ART, CSP, and ART + CSP to analyze cytotoxicity, genotoxicity, cell migration, and increased expression of proteins related to apoptosis and ICD. Additionally, 41 mice were induced with OL using 4NQO, treated with ART and CSP, and their tongues were histologically analyzed.

Results

In vitro, CSP and CSP + ART showed dose-dependent cytotoxicity and reduced SCC-180 migration. No treatment was genotoxic, and none induced expression of proteins related to apoptosis and ICD; CSP considerably reduced High-mobility group box-1 (HMGB-1) protein expression in SCC-180. In vivo, there was a delay in OL progression with ART and CSP treatment; however, by the 16th week, only CSP prevented progression to OSCC.

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