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从淋巴结中扩增肺癌衍生的播散癌细胞,鉴定与转移进展相关的细胞。

Ex vivo expansion of lung cancer-derived disseminated cancer cells from lymph nodes identifies cells associated with metastatic progression.

机构信息

Fraunhofer Institute for Toxicology and Experimental Medicine, Division of Personalized Tumor Therapy, Regensburg, Germany.

Experimental Medicine and Therapy Research, University of Regensburg, Regensburg, Germany.

出版信息

Int J Cancer. 2023 Nov 15;153(10):1854-1867. doi: 10.1002/ijc.34658. Epub 2023 Aug 9.

DOI:10.1002/ijc.34658
PMID:37555668
Abstract

The cellular basis of the apparent aggressiveness in lung cancer is poorly understood but likely associated with functional or molecular features of disseminated cancer cells (DCCs). DCCs from epithelial cancers are mostly detected by antibodies directed against histogenetic markers such as cytokeratin or EpCAM. It has been argued that marker-negative metastatic founder cells might escape detection. We therefore used ex vivo sphere formation for functional detection of candidate metastasis founders. We generated cell suspensions from 199 LN samples of 131 lung cancer patients and placed them into non-adherent cell culture. Sphere formation was associated with detection of DCCs using EpCAM immunocytology and with significantly poorer prognosis. The prognostic impact of sphere formation was strongly associated with high numbers of EpCAM-positive DCCs and aberrant genotypes of expanded spheres. We also noted sphere formation in patients with no evidence of lymphatic spread, however such spheres showed infrequent expression of signature genes associated with spheres from EpCAM-positive samples and displayed neither typical lung cancer mutations (KRAS, TP53, ERBB1) nor copy number variations, but might be linked to disease progression >5 years post curative surgery. We conclude that EpCAM identifies relevant disease-driving DCCs, that such cells can be expanded for model generation and that further research is needed to clarify the functional and prognostic role of rare EpCAM-negative sphere forming cells.

摘要

肺癌明显侵袭性的细胞基础理解甚少,但可能与播散性癌细胞(DCC)的功能或分子特征有关。上皮性癌症的 DCC 主要通过针对细胞角蛋白或 EpCAM 等组织发生标记物的抗体来检测。有人认为,标记阴性的转移性起始细胞可能逃避检测。因此,我们使用体外球体形成来对候选转移起始细胞进行功能检测。我们从 131 例肺癌患者的 199 个淋巴结样本中生成细胞悬浮液,并将其置于非粘附细胞培养中。球体形成与 EpCAM 免疫细胞化学检测到 DCC 有关,并且与预后显著较差有关。球体形成的预后影响与 EpCAM 阳性 DCC 的高数量和扩展球体的异常基因型强烈相关。我们还注意到在没有淋巴扩散证据的患者中也形成了球体,但是这些球体很少表达与 EpCAM 阳性样本球体相关的特征基因,并且既没有典型的肺癌突变(KRAS、TP53、ERBB1),也没有拷贝数变异,但可能与根治性手术后 5 年以上的疾病进展有关。我们得出结论,EpCAM 可识别相关的疾病驱动性 DCC,可对这些细胞进行扩展以用于模型生成,需要进一步研究以阐明罕见的 EpCAM 阴性球体形成细胞的功能和预后作用。

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