Unit of Cancer Genetics, National Research Council (CNR), Institute of Biomolecular Chemistry (ICB), Traversa La Crucca 3, Baldinca Li Punti, 07100, Sassari, Italy.
PAPA GIOVANNI XXIII Cancer Center Hospital, Bergamo, Italy.
Curr Oncol Rep. 2018 Sep 14;20(11):86. doi: 10.1007/s11912-018-0733-7.
Conventional clinico-pathological features in melanoma patients should be integrated with new molecular diagnostic, predictive, and prognostic factors coming from the expanding genomic profiles. Cutaneous melanoma (CM), even differing in biological behavior according to sun-exposure levels on the skin areas where it arises, is molecularly heterogeneous. The next-generation sequencing (NGS) approaches are providing data on mutation landscapes in driver genes that may account for distinct pathogenetic mechanisms and pathways. The purpose was to group and classify all somatic driver mutations observed in the main NGS-based studies.
Whole exome and whole genome sequencing approaches have provided data on spectrum and distribution of genetic and genomic alterations as well as allowed to discover new cancer genes underlying CM pathogenesis. After evaluating the mutational status in a cohort of 686 CM cases from the most representative NGS studies, three molecular CM subtypes were proposed: BRAF, RAS, and non-BRAF/non-RAS.
黑色素瘤患者的传统临床病理特征应与新的分子诊断、预测和预后因素相结合,这些因素来自不断扩展的基因组图谱。皮肤黑色素瘤(CM),即使根据其发生部位皮肤的日晒水平在生物学行为上有所不同,但其分子也是异质的。下一代测序(NGS)方法提供了有关驱动基因中突变景观的数据,这些数据可能解释了不同的发病机制和途径。目的是对主要基于 NGS 的研究中观察到的所有体细胞驱动突变进行分组和分类。
全外显子组和全基因组测序方法提供了有关遗传和基因组改变的范围和分布的数据,并允许发现导致 CM 发病机制的新癌症基因。在评估了来自最具代表性的 NGS 研究的 686 例 CM 病例的突变状态后,提出了三种分子 CM 亚型:BRAF、RAS 和非 BRAF/非 RAS。
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