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Biomarkers as Key Contributors in Treating Malignant Melanoma Metastases

机译:生物标志物作为治疗恶性黑色素瘤转移的关键因素

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Melanoma is a human neurocristopathy associated with developmental defects in the neural crest-derived epidermal melanocytes. At the present time, at least three hypotheses were identified that may explain melanoma aetiology, as follows: (1) a model of linear progression from differentiated melanocytes to metastatic cancer cells (2) a model involving the appearance of melanoma stem-like cells, and (3) an epigenetic progenitor model of cancer. Treating metastatic melanoma is one of the most serious challenges in the 21st century. This is justified because of a subpopulation of cells presenting a remarkable molecular heterogeneity, which is able to explain the drug resistance and the growing mortality rates worldwide. Fortunately, there are now evidences sustaining the importance of genetic, epigenetic, and metabolomic alterations as biomarkers for classification, staging, and better management of melanoma patients. To illustrate some fascinating insights in this field, the genesBRAFV600EandCTLA4have been recognized as bona fide targets to benefit melanoma patients. Our research attempts to carefully evaluate data from the literature in order to highlight the link between a molecular disease model and the key contribution of biomarkers in treating malignant melanoma metastases.
机译:黑色素瘤是与神经rest衍生的表皮黑素细胞发育缺陷相关的人类神经病变。目前,至少确定了三种可能解释黑素瘤病因的假说,如下:(1)从分化的黑素细胞向转移性癌细胞线性发展的模型(2)涉及黑素瘤干细胞样细胞出现的模型, (3)癌症的表观遗传祖细胞模型。治疗转移性黑色素瘤是21世纪最严重的挑战之一。这是有道理的,因为存在大量分子异质性的细胞亚群可以解释耐药性和全球死亡率的上升。幸运的是,现在有证据支持遗传,表观遗传和代谢组学改变作为生物标志物对黑素瘤患者进行分类,分期和更好管理的重要性。为了说明该领域的一些有趣见解,已将基因BRAFV600E和CTLA4视为使黑素瘤患者受益的真正靶标。我们的研究试图仔细评估来自文献的数据,以强调分子疾病模型与生物标志物在治疗恶性黑色素瘤转移中的关键作用之间的联系。

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