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首页> 美国卫生研究院文献>American Journal of Cancer Research >Cisplatin sensitivity mediated by NKX2-1 in lung adenocarcinoma is dependent on p53 mutational status via modulating TNFSF10 expression
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Cisplatin sensitivity mediated by NKX2-1 in lung adenocarcinoma is dependent on p53 mutational status via modulating TNFSF10 expression

机译:NKX2-1介导的肺腺癌顺铂敏感性通过调节TNFSF10表达而依赖于p53突变状态

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NKX2-1 was shown to enhance cisplatin sensitivity in KRAS-mutated cells, but it conferred cisplatin resistance in EGFR-mutated lung adenocarcinoma cells. However, NKX2-1 as a dual role in tumor progression depended on p53 mutational status via modulation of the NF-κB pathway. We hypothesized that NKX2-1 may confer cisplatin resistance in p53-mutated (p53-MT) lung adenocarcinoma cells but may enhance cisplatin sensitivity in wild-type (p53-WT) cells. In the present study, six p53-MT and -p53-WT cell lines were treated with various concentrations of cisplatin to calculate the inhibitory concentration of cisplatin for 50% cell viability (IC ). The IC value was positively correlated with NKX2-1 expression in the p53-MT cells but negatively correlated in the p53-WT cells. TNFSF10 was identified in a microarray analysis as a potential candidate responsible for NKX2-1-mediated apoptosis induced by cisplatin. The retrospective study evaluated 97 surgically resected lung adenocarcinoma patients receiving cisplatin-based chemotherapy to explore the possible association between NKX2-1 expression and tumor response. Patients with higher TNFSF10 mRNA levels, as determined by real-time reverse transcription-polymerase Chain Reaction (RT-PCR), typically showed an favorable response when compared with patients with lower TNFSF10 mRNA levels. Additionally, the association of higher TNFSF10 mRNA levels with favorable response was only revealed in p53-WT patients, not in p53-MT patients. Higher NKX2-1 mRNA levels were associated with an unfavorable response in patients with p53-MT tumors but a favorable response in patients with p53-WT tumors. In summary, modulation of TNFSF10 expression by NKX2-1 may be a potential indicator for predicting the response to cisplatin-based chemotherapy in patients with lung adenocarcinomas.
机译:NKX2-1在KRAS突变的细胞中显示出增强顺铂敏感性的作用,但在EGFR突变的肺腺癌细胞中赋予了顺铂耐药性。然而,NKX2-1在肿瘤进展中起双重作用,取决于通过调节NF-κB途径的p53突变状态。我们假设NKX2-1可能在p53突变的(p53-MT)肺腺癌细胞中赋予顺铂耐药性,但在野生型(p53-WT)的细胞中可能增强顺铂敏感性。在本研究中,用不同浓度的顺铂处理了六个p53-MT和-p53-WT细胞系,以计算出顺铂对50%细胞存活率(IC)的抑制浓度。 IC值与p53-MT细胞中NKX2-1表达呈正相关,而与p53-WT细胞中呈负相关。在微阵列分析中,TNFSF10被确定为负责由顺铂诱导的NKX2-1介导的细胞凋亡的潜在候选者。这项回顾性研究评估了97例接受顺铂化疗的手术切除的肺腺癌患者,以探讨NKX2-1表达与肿瘤反应之间的可能联系。通过实时逆转录聚合酶链反应(RT-PCR)确定的TNFSF10 mRNA水平较高的患者,与TNFSF10 mRNA水平较低的患者相比,通常表现出良好的反应。另外,仅在p53-WT患者中发现较高的TNFSF10 mRNA水平与良好应答相关,而在p53-MT患者中未发现。较高的NKX2-1 mRNA水平与p53-MT肿瘤患者的不良反应相关,而对p53-WT肿瘤患者的不良反应相关。总之,NKX2-1对TNFSF10表达的调节可能是预测肺腺癌患者对基于顺铂化疗的反应的潜在指标。

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