黑色素瘤进展中的上皮-间质转化:受体蛋白ruk / cin85的作用

B. V. Zhuravel
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引用次数: 0

摘要

本研究的目的是验证黑色素瘤细胞中Ruk/CIN85过表达/敲低可能参与EMT调控的假设。材料和方法。以早期利用慢病毒技术生成的Ruk/CIN85上调/下调的小鼠黑色素瘤细胞系B16-F10及其亚系为模型进行研究。在标准条件下,在完整的RPMI 1610培养基中培养黑色素瘤细胞。使用mtt试验估计细胞的增殖活性,并通过伤口愈合试验研究细胞的迁移潜力。所得数据采用参数Student 's t检验进行分析。结果以mean±SEM表示,P<0.05为显著性。结果和讨论。皮肤黑色素瘤的发生是一个多步骤的过程,由正常黑素细胞在癌性损伤后的转化所启动。由于EMT过程中的转录组和代谢组重编程,转化的黑色素瘤细胞改变其表型,获得更高的增殖率、细胞运动性、侵袭性和转移潜力。根据获得的数据,在B16小鼠黑色素瘤细胞(Up7和Up21亚克隆)中,Ruk/CIN85的过表达导致其增殖活性在24小时时比对照Mock细胞分别增加了1倍,6倍和1.8倍。48h,细胞到达汇合时,亚克隆的细胞活力与对照没有差异。抑制接头蛋白(Down亚克隆)表达后,B16细胞的增殖活性无显著变化。根据之前的数据,过表达Ruk/CIN85的B16细胞的特征是运动率显著增加(Up7和Up21亚克隆与对照Mock细胞相比,运动率都增加了两倍以上)。同时,在B16细胞中敲低Ruk/CIN85导致其迁移活性降低约30%。结论。所有研究结果表明,黑素瘤B16细胞的恶性性状随受体蛋白Ruk/CIN85表达水平的变化而呈负调节,提示其可能在EMT的控制中起作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
EPITHELIAL-MESENCHYMAL TRANSITION IN MELANOMA PROGRESSION: THE CONTRIBUTION OF ADAPTOR PROTEIN RUK/CIN85
The purpose of this study was to test the hypothesis that Ruk/CIN85 overexpression/knockdown in melanoma cells may be involved in the regulation of EMT. Materials and methods. The mouse melanoma cell line B16-F10 and its sublines with up-/down-regulation of Ruk/CIN85 (generated early using lentiviral technology) were used as a model for research. Melanoma cells were cultured in the complete RPMI 1610 medium under standard conditions. Proliferative activity of the cells was estimated using the MTT-test, and cell migratory potential was studied by the wound-healing assay. The data obtained were analyzed with parametric Student`s t-test. Results were expressed as mean ± SEM and significance was set at P<0.05. Results and Discussion. Cutaneous melanoma genesis is a multi-step process initiated by the transformation of a normal melanocyte following an oncogenic insult. Due to the transcriptome and metabolome reprogramming in the course of EMT, transformed melanoma cells change their phenotype and acquire increased proliferative rate, cell motility, invasiveness, and metastatic potential. According to the data obtained, overexpression of Ruk/CIN85 in B16 mouse melanoma cells (subclones Up7 and Up21) led to an increase in their proliferative activity by 1,6 and 1.8 times, respectively, at 24th hour in comparison with control Mock cells . At the 48th hour, when the cells reached confluence, the cell viability of subclones did not differ from the control ones. No statistically significant changes in the proliferative activity of B16 cells with suppressed expression of the adaptor protein (subclone Down) were found. In accordance with previous data, B16 cells overexpressing Ruk/CIN85 were characterized by strongly increased motility rate (more than twofold for both Up7 and Up21 subclones compared to control Mock cells). At the same time, knockdown of Ruk/CIN85 in B16 cells resulted in a decrease in their migratory activity by about 30%. Conclusions. All findings obtained demonstrated that the malignancy traits of melanoma B16 cells are inversely modulated upon up- and down-changes in adaptor protein Ruk/CIN85 expression levels suggesting its possible role in the control of EMT.
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