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MYCN downregulates integrin α1 to promote invasion of human neuroblastoma cells

机译:MYCN下调整联蛋白α1促进人神经母细胞瘤细胞的侵袭

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Neuroblastoma is a childhood tumor thought to arise through improper differentiation of neural crest cells. MYCN amplification is a prognostic factor that indicates a highly malignant disease and poor patient prognosis. Integrins are important regulators of neuroblastoma attachment and migration and participate in many aspects of metastasis. However, the role of integrins in neuroblastoma metastasis, the leading cause of death from this disease, remains less well understood. Screening of neuroblastoma cell lines for integrin mRNA expression showed that integrin α1 expression was higher in lines such as SK-N-SH and NB69 that do not have MYCN amplification than in cell lines such as IMR32, NB1, NB9 and NB19 that have MYCN amplification. A knockdown of MYCN in NB1 and NB19 cells resulted in increased expression of integrin α1, which correlated with enhanced attachment to the extracellular matrix and reduced migratory activity. In contrast, the overexpression of MYCN in SK-N-SH and NB69 cells resulted in decreased expression of integrin α1, which correlated with reduced attachment to the extracellular matrix and enhanced migratory activity. These results show that MYCN may limit cell adhesion to the extracellular matrix and promote cell migration by downregulating integrin α1.
机译:神经母细胞瘤是一种儿童肿瘤,被认为是由于神经c细胞的不适当分化而引起的。 MYCN扩增是预后因素,表明高度恶性疾病和较差的患者预后。整联蛋白是神经母细胞瘤附着和迁移的重要调节剂,并参与转移的许多方面。然而,整联蛋白在神经母细胞瘤转移中的作用,这种疾病的主要死因仍不清楚。对成胶质细胞mRNA表达的神经母细胞瘤细胞系的筛选显示,在不具有MYCN扩增的细胞系(例如SK-N-SH和NB69)中,在具有MYCN扩增的细胞系(例如IMR32,NB1,NB9和NB19)中,整合素α1表达更高。敲低NB1和NB19细胞中的MYCN导致整合素α1的表达增加,这与增强对细胞外基质的附着和降低的迁移活性相关。相反,MYCN在SK-N-SH和NB69细胞中的过表达导致整合素α1的表达降低,这与减少对细胞外基质的附着和增强的迁徙活性相关。这些结果表明,MYCN可能通过下调整联蛋白α1来限制细胞对细胞外基质的粘附并促进细胞迁移。

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