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A rare subpopulation of melanoma cells with low expression of metastasis suppressor NME1 is highly metastatic in vivo

机译:具有低表达转移抑制器NME1的黑色素瘤细胞的稀有亚群是体内高度转移的

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Despite recent advances in melanoma treatment, metastasis and resistance to therapy remain serious clinical challenges. NME1 is a metastasis suppressor, a class of proteins which inhibits metastatic spread of cancer cells without impact on growth of the primary tumor. We have identified a rare subpopulation of cells with markedly reduced expression of NME1 (NME1LOW) in human melanoma cell lines. To enable isolation of viable NME1LOW cells for phenotypic analysis by fluorescence-activated cell sorting (FACS), a CRISPR-Cas9-mediated approach was used to attach an EGFP coding module to the C-terminus of the endogenous NME1 gene in melanoma cell lines. NME1LOW cells displayed enhanced collective invasion in vitro when implanted as 3D aggregates in Matrigel. NME1LOW cells were also highly metastatic to lung and liver when xenografted subcutaneously in immune-deficient NSG mice. RNA-seq analysis revealed that NME1LOW cells express elevated levels of genes associated with tumor aggressiveness, as well as with morphogenesis of tissues of neural crest-like origin (melanocytes and neurons, bone and heart tissues; GO: 0009653). The highly malignant NME1LOW variant of melanoma cells has potential to provide novel therapeutic targets and molecular markers for improved clinical management of patients with advanced melanoma.
机译:尽管最近的黑色素瘤治疗,转移和对治疗的抗性仍然是严重的临床挑战。 NME1是一种转移抑制剂,一类抑制癌细胞转移扩散而不会影响原发性肿瘤的生长。我们已经确定了具有显着降低人黑素瘤细胞系中NME1(NME1LOW)的细胞的罕见亚群。为了能够通过荧光激活的细胞分选(FACS)分离用于表型分析的活性NME1LOW细胞,使用CRISPR-CAS9介导的方法将EGFP编码模块与黑素瘤细胞系中内源NME1基因的C-末端附着。当Matrigel中的3D聚集体植入时,NME1LOW细胞在体外显示增强的集体侵袭。当在免疫缺陷的NSG小鼠中皮下切割出异种移植时,NME1LOW细胞对肺和肝脏的高度转移。 RNA-SEQ分析显示,NME1LOW细胞表达升高的基因水平与肿瘤侵蚀性相关的基因,以及神经嵴起源组织的形态发生(黑色细胞和神经元,骨骼和心脏组织; GO:0009653)。黑素瘤细胞的高度恶性NME1LOW变体具有提供新的治疗靶标和分子标志物,用于改善先进黑素瘤患者的临床管理。

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