皮肤黑色素瘤的基因组分类
Genomic Classification of Cutaneous Melanoma.
出版信息
Cell. 2015 Jun 18;161(7):1681-96. doi: 10.1016/j.cell.2015.05.044.
Abstract
We describe the landscape of genomic alterations in cutaneous melanomas through DNA, RNA, and protein-based analysis of 333 primary and/or metastatic melanomas from 331 patients. We establish a framework for genomic classification into one of four subtypes based on the pattern of the most prevalent significantly mutated genes: mutant BRAF, mutant RAS, mutant NF1, and Triple-WT (wild-type). Integrative analysis reveals enrichment of KIT mutations and focal amplifications and complex structural rearrangements as a feature of the Triple-WT subtype. We found no significant outcome correlation with genomic classification, but samples assigned a transcriptomic subclass enriched for immune gene expression associated with lymphocyte infiltrate on pathology review and high LCK protein expression, a T cell marker, were associated with improved patient survival. This clinicopathological and multi-dimensional analysis suggests that the prognosis of melanoma patients with regional metastases is influenced by tumor stroma immunobiology, offering insights to further personalize therapeutic decision-making.
摘要
我们通过对来自331名患者的333例原发性和/或转移性黑色素瘤进行基于DNA、RNA和蛋白质的分析,描述了皮肤黑色素瘤的基因组改变情况。我们基于最常见的显著突变基因模式,建立了一个基因组分类框架,将其分为四种亚型之一:BRAF突变型、RAS突变型、NF1突变型和三野生型(野生型)。综合分析显示,KIT突变、局部扩增和复杂结构重排的富集是三野生型亚型的一个特征。我们发现基因组分类与预后无显著相关性,但在病理检查中,转录组亚类富含与淋巴细胞浸润相关的免疫基因表达且高表达T细胞标志物LCK蛋白的样本,与患者生存率提高相关。这种临床病理和多维度分析表明,伴有区域转移的黑色素瘤患者的预后受肿瘤基质免疫生物学影响,为进一步个性化治疗决策提供了见解。
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