Molecular Oncology Laboratory, Fundación Hospital General Universitario de Valencia, Valencia, Spain.
CIBERONC, Valencia, Spain.
Cell Death Dis. 2019 Sep 10;10(9):660. doi: 10.1038/s41419-019-1898-1.
The high resistance against current therapies found in non-small-cell lung cancer (NSCLC) has been associated to cancer stem-like cells (CSCs), a population for which the identification of targets and biomarkers is still under development. In this study, primary cultures from early-stage NSCLC patients were established, using sphere-forming assays for CSC enrichment and adherent conditions for the control counterparts. Patient-derived tumorspheres showed self-renewal and unlimited exponential growth potentials, resistance against chemotherapeutic agents, invasion and differentiation capacities in vitro, and superior tumorigenic potential in vivo. Using quantitative PCR, gene expression profiles were analyzed and NANOG, NOTCH3, CD44, CDKN1A, SNAI1, and ITGA6 were selected to distinguish tumorspheres from adherent cells. Immunoblot and immunofluorescence analyses confirmed that proteins encoded by these genes were consistently increased in tumorspheres from adenocarcinoma patients and showed differential localization and expression patterns. The prognostic role of genes significantly overexpressed in tumorspheres was evaluated in a NSCLC cohort (N = 661) from The Cancer Genome Atlas. Based on a Cox regression analysis, CDKN1A, SNAI1, and ITGA6 were found to be associated with prognosis and used to calculate a gene expression score, named CSC score. Kaplan-Meier survival analysis showed that patients with high CSC score have shorter overall survival (OS) in the entire cohort [37.7 vs. 60.4 months (mo), p = 0.001] and the adenocarcinoma subcohort [36.6 vs. 53.5 mo, p = 0.003], but not in the squamous cell carcinoma one. Multivariate analysis indicated that this gene expression score is an independent biomarker of prognosis for OS in both the entire cohort [hazard ratio (HR): 1.498; 95% confidence interval (CI), 1.167-1.922; p = 0.001] and the adenocarcinoma subcohort [HR: 1.869; 95% CI, 1.275-2.738; p = 0.001]. This score was also analyzed in an independent cohort of 114 adenocarcinoma patients, confirming its prognostic value [42.90 vs. not reached (NR) mo, p = 0.020]. In conclusion, our findings provide relevant prognostic information for lung adenocarcinoma patients and the basis for developing novel therapies. Further studies are required to identify suitable markers and targets for lung squamous cell carcinoma patients.
非小细胞肺癌 (NSCLC) 对当前治疗方法的高耐药性与癌症干细胞样细胞 (CSC) 有关,目前仍在开发针对这些细胞的靶点和生物标志物。在这项研究中,使用球体形成实验富集 CSC 并在贴壁条件下培养对照细胞,从而建立了来自早期 NSCLC 患者的原代培养物。患者来源的肿瘤球具有自我更新和无限的指数增长潜力、对化疗药物的耐药性、体外侵袭和分化能力,以及体内更高的致瘤能力。通过定量 PCR 分析基因表达谱,选择 NANOG、NOTCH3、CD44、CDKN1A、SNAI1 和 ITGA6 来区分肿瘤球和贴壁细胞。免疫印迹和免疫荧光分析证实,这些基因编码的蛋白在腺癌患者的肿瘤球中持续增加,并显示出不同的定位和表达模式。在癌症基因组图谱 (TCGA) 的 NSCLC 队列 (N=661) 中评估了在肿瘤球中显著过表达的基因的预后作用。基于 Cox 回归分析,CDKN1A、SNAI1 和 ITGA6 与预后相关,并用于计算基因表达评分,命名为 CSC 评分。Kaplan-Meier 生存分析显示,高 CSC 评分患者的总生存期 (OS) 在整个队列中较短[37.7 与 60.4 个月 (mo),p=0.001]和腺癌亚组[36.6 与 53.5 mo,p=0.003],但在鳞癌亚组中则不然。多变量分析表明,该基因表达评分是 OS 的独立预后生物标志物,在整个队列 [风险比 (HR):1.498;95%置信区间 (CI),1.167-1.922;p=0.001] 和腺癌亚组 [HR:1.869;95%CI,1.275-2.738;p=0.001] 中均如此。在另一个包含 114 名腺癌患者的独立队列中分析了该评分,证实了其预后价值[42.90 与未达到 (NR) mo,p=0.020]。总之,我们的研究结果为肺腺癌患者提供了相关的预后信息,并为开发新的治疗方法奠定了基础。需要进一步的研究来确定肺鳞癌患者合适的标志物和靶点。
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