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N-Myc knockdown and apigenin treatment controlled growth of malignant neuroblastoma cells having N-Myc amplification

机译:N-Myc抑制和芹菜素处理可控制具有N-Myc扩增的恶性成神经细胞瘤细胞的生长

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Malignant neuroblastomas mostly occur in children and are frequently associated with N-Myc amplification. Oncogene amplification, which is selective increase in copy number of the oncogene, provides survival advantages in solid tumors including malignant neuroblastoma. We have decreased expression of N-Myc oncogene using short hairpin RNA (shRNA) plasmid to increase anti-tumor efficacy of the isoflavonoid apigenin (APG) in human malignant neuroblastoma SK-N-DZ and SK-N-BE2 cell lines that harbor N-Myc amplification. N-Myc knockdown induced morphological and biochemical features of neuronal differentiation. Combination of N-Myc knockdown and APG most effectively induced morphological and biochemical features of apoptotic death. This combination therapy also prevented cell migration and decreased N-Myc driven survival, angiogenic, and invasive factors. Collectively, N-Myc knockdown and APG treatment is a promising strategy for controlling the growth of human malignant neuroblastoma cell lines that harbor N-Myc amplification.
机译:恶性神经母细胞瘤多发于儿童,并经常与N-Myc扩增有关。癌基因扩增是癌基因拷贝数的选择性增加,在包括恶性神经母细胞瘤在内的实体瘤中具有生存优势。我们使用短发夹RNA(shRNA)质粒降低了N-Myc癌基因的表达,以增加异黄酮芹菜素(APG)在人类恶性神经母细胞瘤SK-N-DZ和SK-N-BE2细胞株中的抗肿瘤功效-Myc扩增。 N-Myc组合式诱导神经元分化的形态和生化特征。 N-Myc组合和APG的组合最有效地诱导了凋亡死亡的形态和生化特征。这种联合疗法还可以防止细胞迁移并减少N-Myc驱动的存活率,血管生成和侵袭性因子。总而言之,N-Myc抑制和APG治疗是控制具有N-Myc扩增功能的人类恶性神经母细胞瘤细胞系生长的一种有前途的策略。

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