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Melanocytes Affect Nodal Expression and Signaling in Melanoma Cells: A Lesson from Pediatric Large Congenital Melanocytic Nevi

机译:黑色素细胞影响黑色素瘤细胞中的节点表达和信号:儿科大型先天性黑素细胞痣的教训。

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摘要

Expression of Nodal, a Transforming Growth Factor-beta (TGF-β) related growth factor, is associated with aggressive melanoma. Nodal expression in adult dysplastic nevi may predict the development of aggressive melanoma in some patients. A subset of pediatric patients diagnosed with giant or large congenital melanocytic nevi (LCMN) has shown increased risk for development of melanoma. Here, we investigate whether Nodal expression can help identify the rare cases of LCMN that develop melanoma and shed light on why the majority of these patients do not. Immunohistochemistry (IHC) staining results show varying degree of Nodal expression in pediatric dysplastic nevi and LCMN. Moreover, median scores from Nodal IHC expression analysis were not significantly different between these two groups. Additionally, none of the LCMN patients in this study developed melanoma, regardless of Nodal IHC levels. Co-culture experiments revealed reduced tumor growth and lower levels of Nodal and its signaling molecules P-SMAD2 and P-ERK1/2 when melanoma cells were grown in vivo or in vitro with normal melanocytes. The same was observed in melanoma cells cultured with melanocyte conditioned media containing pigmented melanocyte derived melanosomes (MDM). Since MDM contain molecules capable of inactivating radical oxygen species, to investigate potential anti-oxidant effect of MDM on Nodal expression and signaling in melanoma, melanoma cells were treated with either N-acetyl-l-cysteine (NAC), a component of the anti-oxidant glutathione or synthetic melanin, which in addition to providing pigmentation can also exert free radical scavenging activity. Melanoma cells treated with NAC or synthetic melanin showed reduced levels of Nodal, P-SMAD2 and P-ERK1/2 compared to untreated melanoma cells. Thus, the potential role for Nodal in melanoma development in LCMN is less evident than in adult dysplastic nevi possibly due to melanocyte cross-talk in LCMN capable of offsetting or delaying the pro-melanoma effects of Nodal via anti-oxidant effects of MDM.
机译:淋巴结的表达是与转化性生长因子-β(TGF-β)相关的生长因子,与侵袭性黑色素瘤相关。成人发育异常痣中的淋巴结表达可能预示了某些患者中侵袭性黑色素瘤的发展。被诊断出患有巨人或大型先天性黑素细胞痣(LCMN)的小儿科患者的子集显示出患黑色素瘤的风险增加。在这里,我们调查了Nodal的表达是否可以帮助识别罕见的发展为黑色素瘤的LCMN病例,并阐明了为什么大多数这些患者没有。免疫组织化学(IHC)染色结果显示,小儿发育不良痣和LCMN中Nodal表达程度不同。此外,在这两组之间,来自Nodal IHC表达分析的中位数得分没有显着差异。此外,无论Nodal IHC水平如何,本研究中没有LCMN患者发生黑色素瘤。共培养实验表明,当黑素瘤细胞在体内或体外与正常黑素细胞一起生长时,肿瘤的生长减少,Nodal及其信号分子P-SMAD2和P-ERK1 / 2的水平降低。在用含有色素的黑素细胞衍生的黑素体(MDM)的黑素细胞条件培养基培养的黑素瘤细胞中也观察到了同样的情况。由于MDM包含能够灭活自由基氧分子的分子,为了研究MDM对黑色素瘤中Nodal表达和信号转导的潜在抗氧化作用,因此用N-乙酰基-1-半胱氨酸(NAC)处理黑色素瘤细胞, -氧化剂谷胱甘肽或合成的黑色素,除了提供色素沉着外,还可以发挥自由基清除活性。与未处理的黑色素瘤细胞相比,用NAC或合成的黑色素处理的黑色素瘤细胞的Nodal,P-SMAD2和P-ERK1 / 2水平降低。因此,Nodal在LCMN黑色素瘤发展中的潜在作用不如在成年发育不良痣中明显,这可能是由于LCMN中的黑素细胞串扰能够通过MDM的抗氧化作用抵消或延迟Nodal的促黑素瘤作用。

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