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Comparative genomics reveals that loss of lunatic fringe (LFNG) promotes melanoma metastasis

机译:比较基因组学揭示了疯癫条纹(LFNG)的缺失会促进黑色素瘤转移

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摘要

Metastasis is the leading cause of death in patients with advanced melanoma, yet the somatic alterations that aid tumour cell dissemination and colonisation are poorly understood. Here, we deploy comparative genomics to identify and validate clinically relevant drivers of melanoma metastasis. To do this, we identified a set of 976 genes whose expression level was associated with a poor outcome in patients from two large melanoma cohorts. Next, we characterised the genomes and transcriptomes of mouse melanoma cell lines defined as weakly metastatic, and their highly metastatic derivatives. By comparing expression data between species, we identified lunatic fringe (LFNG), among 28 genes whose expression level is predictive of poor prognosis and whose altered expression is associated with a prometastatic phenotype in mouse melanoma cells. CRISPR/Cas9‐mediated knockout of Lfng dramatically enhanced the capability of weakly metastatic melanoma cells to metastasise in vivo, a phenotype that could be rescued with the Lfng cDNA. Notably, genomic alterations disrupting LFNG are found exclusively in human metastatic melanomas sequenced as part of The Cancer Genome Atlas. Using comparative genomics, we show that LFNG expression plays a functional role in regulating melanoma metastasis.
机译:转移是晚期黑色素瘤患者死亡的主要原因,但对有助于肿瘤细胞扩散和定植的体细胞改变了解甚少。在这里,我们采用比较基因组学来识别和验证临床上与黑色素瘤转移相关的驱动因素。为此,我们鉴定了一组976个基因,它们的表达水平与来自两个大型黑色素瘤队列的患者预后不良有关。接下来,我们表征了被定义为弱转移的小鼠黑素瘤细胞系的基因组和转录组,以及它们高度转移的衍生物。通过比较物种之间的表达数据,我们在表达水平可预测不良预后并且其表达改变与小鼠黑色素瘤细胞表型相关的28个基因中鉴定出了疯人条纹(LFNG)。 CRISPR / Cas9介导的Lfng敲除显着增强了弱转移黑色素瘤细胞在体内转移的能力,该表型可以通过Lfng cDNA挽救。值得注意的是,破坏LFNG的基因组改变仅在作为癌症基因组图谱一部分进行测序的人类转移性黑色素瘤中发现。使用比较基因组学,我们显示LFNG表达在调节黑色素瘤转移中发挥功能性作用。

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