褪黑素通过细胞周期阻滞和细胞骨架重塑抑制人类黑色素瘤细胞的增殖和侵袭

A. C. R. Moreno, R. F. Saito, Manoela Tiago, R. R. Massaro, R. Pagni, Rafael Pegoraro, Patrícia da Cruz Souza, R. Reiter, A. Campa, M. Soengas, S. Maria-Engler
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引用次数: 9

摘要

在皮肤癌中,黑色素瘤的死亡率最高。异质性遗传黑素瘤背景导致肿瘤传播能力在维持治疗耐药性和肿瘤复发中尤为重要。能够控制黑色素瘤进展的有效分子的识别代表了新的治疗策略的重要机会,特别是与当前的标准治疗相结合。在此背景下,一些研究报道了褪黑素对不同类型癌症的抗肿瘤作用,包括黑色素瘤。在这里,我们描述了与褪黑素在人类黑色素瘤细胞系中的活性相关的潜在机制,重点是细胞周期和细胞骨架重塑。有趣的是,当褪黑素诱导黑素细胞DNA复制时,黑色素瘤细胞在g1期表现出细胞周期阻滞。这种现象与cyclin-D1下调或p21过表达有关。褪黑素对黑色素瘤细胞存活和增殖的影响是通过克隆生成实验检测的,菌落的数量和大小都有所减少。此外,褪黑素在所有黑色素瘤细胞系中诱导了戏剧性的细胞骨架重塑,导致星形形态或细胞肿胀。褪黑素对黑色素瘤细胞骨架的作用与肌动蛋白破坏、肌动蛋白纤维变薄和/或断裂以及沿应力纤维的paxillin变弱和/或丢失有关。这些数据支持了褪黑素在皮肤重建模型中损害黑色素瘤侵袭的观察结果。总之,我们的研究结果表明,褪黑素可以用来控制黑色素瘤的生长,并支持褪黑素作为黑色素瘤治疗中有前途的免疫代谢辅助剂的基础和临床研究。
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Melatonin inhibits human melanoma cells proliferation and invasion via cell cycle arrest and cytoskeleton remodeling
Among skin cancers, melanoma has the highest mortality rate. The heterogeneous genetic melanoma background leads to a tumor-propagating capacity particularly important in maintaining therapeutic resistance, and tumor recurrence. The identification of efficient molecules able to control melanoma progress represents an important opportunity for new therapeutic strategies, particularly in combination with the current standard-of-care treatments. In this context, several studies have reported the antitumor effects of melatonin against different types of cancer, including melanoma. Here, we describe the underlying mechanisms associated with melatonin’s activity in human melanoma cell lines, focusing on cell cycle and cytoskeleton remodeling. Interestingly, while melatonin induced melanocyte DNA replication, melanoma cells exhibited cell cycle arrest in the G1-phase. This phenomenon was associated with cyclin-D1 downregulation or p21 overexpression. The efficacy of melatonin on melanoma cells survival and proliferation was detected using the clonogenic assay, with a decrease in both the number and size of colonies. Additionally, melatonin induced a dramatic cytoskeleton remodeling in all melanoma cell lines, leading to a star-like morphology or cell swelling. The role of melatonin on melanoma cytoskeleton was associated with the actin disruption, with thinning and/or broken actin fibers, and weak and/or loss of paxillin along stress fibers. These data support the observed findings that melatonin impairs melanoma invasion in skin reconstructed models. Together, our results suggest that melatonin could be used to control melanoma growth and support basic and clinical studies on melatonin as a promising immunometabolic adjuvant for melanoma therapy.
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