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首页> 外文期刊>Melanoma research >C-Met, epidermal growth factor receptor, and insulin-like growth factor-1 receptor are important for growth in uveal melanoma and independently contribute to migration and metastatic potential
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C-Met, epidermal growth factor receptor, and insulin-like growth factor-1 receptor are important for growth in uveal melanoma and independently contribute to migration and metastatic potential

机译:C-Met,表皮生长因子受体和胰岛素样生长因子-1受体对于葡萄膜黑色素瘤的生长很重要,并独立地促进迁移和转移潜力

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Uveal melanoma (UM) has a high propensity to develop hepatic metastases. We sought to define the mechanisms required for preferential liver homing and to understand further the biologic behavior of this disease. The Met tyrosine kinase receptor and its ligand hepatocyte growth factor are expressed in hepatocytes. We therefore considered Met/hepatocyte growth factor signaling as a candidate migration/growth factor for UM cells. We further explored the relationship between c-Met and other growth factor receptors prevalent in the liver and their roles in UM metastatic potential. UM cell lines were evaluated for c-Met, epidermal growth factor receptor (EGFR), and insulin-like growth factor-1R (IGF-1R) expression by immunoblotting, and gene amplification by comparative genomic hybridization and fluorescence in-situ hybridization. High c-Met, phosphorylated c-Met, and EGFR expression were noted in two of nine cell lines, independent of IGF-1R levels. Knockdown of c-Met decreased proliferation of high c-Met-expressing UM cells but did not induce apoptosis. Selective inhibitors of EGFR and IGF-1R decreased proliferation and induced apoptosis in UM cells regardless of the expression levels of c-Met, EGFR, and IGF-1R. Although c-Met, EGFR, and IGF-1R play proliferative roles, EGFR and IGF-1R are also critical for UM cell survival. High c-Met/EGFR-expressing cell lines possessed the greatest migration potential. c-Met knockdown and selective inhibitors of c-Met, EGFR, and IGF-1R revealed independent contribution of these receptors to migration. UM can be categorized by levels of c-Met and EGFR expression which are associated with migratory/invasiveness responses to soluble factors present at high levels in the liver. This provides biologic relevance for UM clinical behavior with potential therapeutic implications. Melanoma Res 22:123-132
机译:葡萄膜黑色素瘤(UM)具有发展为肝转移的高倾向。我们试图定义优先肝归巢所需的机制,并进一步了解这种疾病的生物学行为。 Met酪氨酸激酶受体及其配体肝细胞生长因子在肝细胞中表达。因此,我们认为Met /肝细胞生长因子信号传导是UM细胞的候选迁移/生长因子。我们进一步探讨了c-Met与肝脏中普遍存在的其他生长因子受体之间的关系及其在UM转移潜能中的作用。通过免疫印迹评估UM细胞系的c-Met,表皮生长因子受体(EGFR)和胰岛素样生长因子-1R(IGF-1R)表达,并通过比较基因组杂交和荧光原位杂交评估基因扩增。在九个细胞系中的两个中,注意到高的c-Met,磷酸化的c-Met和EGFR表达,而与IGF-1R水平无关。击倒c-Met可降低高表达c-Met的UM细胞的增殖,但不会诱导细胞凋亡。不论c-Met,EGFR和IGF-1R的表达水平如何,EGFR和IGF-1R的选择性抑制剂均可降低UM细胞的增殖并诱导其凋亡。尽管c-Met,EGFR和IGF-1R发挥增殖作用,但EGFR和IGF-1R对UM细胞存活也至关重要。高表达c-Met / EGFR的细胞系具有最大的迁移潜力。 c-Met基因敲低和c-Met,EGFR和IGF-1R的选择性抑制剂揭示了这些受体对迁移的独立贡献。 UM可以按c-Met和EGFR表达水平进行分类,这些水平与肝脏中高水平存在的可溶性因子的迁移/侵袭反应有关。这为UM临床行为提供了生物学相关性,并具有潜在的治疗意义。黑色素瘤研究22:123-132

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