Intratumoral injection of melatonin enhances tumor regression in cell line-derived and patient-derived xenografts of head and neck cancer by increasing mitochondrial oxidative stress

褪黑素 医学 头颈部鳞状细胞癌 转移 体内 癌症 头颈部癌 细胞凋亡 癌症研究 顺铂 佐剂 氧化应激 肿瘤进展 内科学 肿瘤科 药理学 化疗 生物 生物化学 生物技术
作者
Laura Martinez‐Ruiz,Javier Florido,César Rodríguez-Santana,Alba López‐Rodríguez,Ana Guerra‐Librero,Beatriz I. Fernández-Gil,Patricia García-Tárraga,José Manuel García‐Verdugo,Felix Oppel,Holger Sudhoff,David Sánchez‐Porras,Amadeo Ten‐Esteve,José Fernández‐Martínez,Pilar González-García,Iryna Rusanova,Darío Acuña‐Castroviejo,Víctor Carriel,Germaine Escames
出处
期刊:Biomedicine & Pharmacotherapy [Elsevier BV]
卷期号:167: 115518-115518 被引量:10
标识
DOI:10.1016/j.biopha.2023.115518
摘要

Head and neck squamous cell carcinoma present a high mortality rate. Melatonin has been shown to have oncostatic effects in different types of cancers. However, inconsistent results have been reported for in vivo applications. Consequently, an alternative administration route is needed to improve bioavailability and establish the optimal dosage of melatonin for cancer treatment. On the other hand, the use of patient-derived tumor models has transformed the field of drug research because they reflect the heterogeneity of patient tumor tissues. In the present study, we explore mechanisms for increasing melatonin bioavailability in tumors and investigate its potential as an adjuvant to improve the therapeutic efficacy of cisplatin in the setting of both xenotransplanted cell lines and primary human HNSCC. We analyzed the effect of two different formulations of melatonin administered subcutaneously or intratumorally in Cal-27 and SCC-9 xenografts and in patient-derived xenografts. Melatonin effects on tumor mitochondrial metabolism was also evaluated as well as melatonin actions on tumor cell migration. In contrast to the results obtained with the subcutaneous melatonin, intratumoral injection of melatonin drastically inhibited tumor progression in HNSCC-derived xenografts, as well as in patient-derived xenografts. Interestingly, intratumoral injection of melatonin potentiated CDDP effects, decreasing Cal-27 tumor growth. We demonstrated that melatonin increases ROS production and apoptosis in tumors, targeting mitochondria. Melatonin also reduces migration capacities and metastasis markers. These results illustrate the great clinical potential of intratumoral melatonin treatment and encourage a future clinical trial in cancer patients to establish a proper clinical melatonin treatment.
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