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首页> 外文期刊>Cell death & disease. >1,25-dihydroxyvitamin D3 signaling-induced decreases in IRX4 inhibits NANOG-mediated cancer stem-like properties and gefitinib resistance in NSCLC cells
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1,25-dihydroxyvitamin D3 signaling-induced decreases in IRX4 inhibits NANOG-mediated cancer stem-like properties and gefitinib resistance in NSCLC cells

机译:1,25-二羟基维生素D3信号诱导的IRX4中的降低抑制NSCLC细胞中的纳米介导的癌症状性质和吉替尼电阻

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Recent studies have demonstrated that acquisition of cancer stem-like properties plays an essential role in promoting epidermal growth factor receptor-tyrosine kinase inhibitors (EGFR-TKIs) resistance in non-small cell lung cancer (NSCLC); however, how to regulate cancer stem-like properties and EGFR-TKI resistance is largely unclear. In this study, we discovered that increased iroquois-class homeodomain protein 4 (IRX4) was related to gefitinib resistance in NSCLC cells. Knockdown of IRX4 inhibited cell proliferation, sphere formation, and the expression of CD133, ALDH1A1, NANOG, Sox2 and Notch1, and the transcriptional activity of NANOG promoter. IRX4 overexpression increased the protein level of NANOG and CD133 in PC-9 cells. Combination of knocking-down IRX4 with gefitinib increased cell apoptosis and decreased cell viability and the expression of p-EGFR and NANOG in PC-9/GR cells. IRX4 knockdown in a PC-9/GR xenograft tumor model inhibited tumor progression and the expression of NANOG and CD133 more effectively than single treatment alone. Knockdown of NANOG inhibited the expression of CD133 and restored gefitinib cytotoxicity, and NANOG overexpression-induced cancer stem-like properties and gefitinib resistance could be obviously reversed by knocking-down IRX4. Further, we found that 1,25-dihydroxyvitamin D3 (1,25(OH)2D3) reduced obviously the expression of IRX4 and NANOG by inhibiting the activation of TGF-β1/Smad3 signaling pathway; moreover, combination of 1,25(OH)2D3 and gefitinib decreased cell viability and proliferation or tumor progression and the expression of IRX4 and NANOG compared with single treatment alone both in PC-9/GR cells and in a PC-9/GR xenograft tumor model. These results reveal that inhibition of IRX4-mediated cancer stem-like properties by regulating 1,25(OH)2D3 signaling may increase gefitinib cytotoxicity. Combination therapy of gefitinib and 1,25(OH)2D3 by targeting IRX4 and NANOG, could provide a promising strategy to improve gefitinib cytotoxicity.
机译:最近的研究表明,癌症状性质的获取在促进非小细胞肺癌(NSCLC)中促进表皮生长因子受体 - 酪氨酸激酶抑制剂(EGFR-TKIS)抗性起作用。然而,如何调节癌症干燥的性质和EGFR-TKI抗性在很大程度上不清楚。在这项研究中,我们发现增加的Iroquois-Class Homodomain蛋白4(IRX4)与NSCLC细胞中的吉替尼抗性有关。 IRX4的敲低抑制细胞增殖,球形形成和CD133,AlDH1a1,纳米,SOx2和Notch1的表达,以及纳米促进剂的转录活性。 IRX4过表达增加了PC-9细胞中纳米蛋白水平和CD133。爆震IRX4与吉非替尼增加的细胞凋亡和细胞活力降低以及PC-9 / GR细胞中P-EGFR和纳米的表达的组合。 PC-9 / GR异种移植肿瘤模型中的IRX4敲低抑制肿瘤进展和纳米和CD133的表达,而不是单独的单独治疗。 Nanog的敲低抑制CD133的表达并恢复的吉替尼细胞毒性,并且纳米过表达诱导的癌症状性能和吉替尼抗性可能明显通过敲低IRX4反转。此外,我们发现,通过抑制TGF-β1/ smad3信号传导途径的激活,1,25-二羟基维生素D3(1,25(OH)2D3)显然降低了IRX4和Nano的表达;此外,1,25(OH)2D3和Gefitinib的组合降低了细胞活力和增殖或肿瘤进展以及IRX4和Nanog的表达与单独的PC-9 / GR细胞和PC-9 / GR异种移植物肿瘤模型。这些结果表明,通过调节1,25(OH)2D3信号传导可以增加吉非替尼细胞毒性,抑制IRX4介导的癌症状性能。通过靶向IRX4和Nanog的Gefitinib和1,25(OH)2D3的组合治疗可以提供有希望改善吉替尼细胞毒性的有希望的策略。

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