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Full-length cytokeratin-19 is released by human tumor cells: a potential role in metastatic progression of breast cancer

机译:全长细胞角蛋白19被人类肿瘤细胞释放:在乳腺癌转移进程中的潜在作用

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IntroductionWe evaluated whether CK19, one of the main cytoskeleton proteins of epithelial cells, is released as full-length protein from viable tumor cells and whether this property is relevant for metastatic progression in breast cancer patients.MethodsEPISPOT (EPithelial ImmunoSPOT) assays were performed to analyze the release of full-length CK19 by carcinoma cells of various origins, and the sequence of CK19 was analyzed with mass spectrometry. Additional functional experiments with cycloheximide, Brefeldin A, or vincristine were done to analyze the biology of the CK19-release. CK19-EPISPOT was used to detect disseminated tumor cells in bone marrow (BM) of 45 breast cancer patients who were then followed up over a median of 6 years.ResultsCK19 was expressed and released by colorectal (HT-29, HCT116, Caco-2) and breast (MCF-7, SKBR3, and MDA-MB-231) cancer cell lines. The CK19-EPISPOT was more sensitive than the CK19-ELISA. Dual fluorescent EPISPOT with antibodies against different CK19 epitopes showed the release of the full-length CK19, which was confirmed by mass spectrometry. Functional experiments indicated that CK19 release was an active process and not simply the consequence of cell death. CK19-releasing cells (RCs) were detectable in BM of 44% to 70% of breast cancer patients. This incidence and the number of CK19-RCs were correlated to the presence of overt metastases, and patients with CK19-RCs had a reduced survival as compared with patients without these cells (P = 0.025, log-rank test; P = 0.0019, hazard ratio, 4.7; multivariate analysis).ConclusionsFull-length CK19 is released by viable epithelial tumor cells, and CK19-RCs might constitute a biologically active subset of breast cancer cells with high metastatic properties.
机译:简介我们评估了上皮细胞的主要细胞骨架蛋白之一CK19是否以全长蛋白的形式从存活的肿瘤细胞中释放出来,并且该特性是否与乳腺癌患者的转移进展有关。方法采用EPISPOT(EPithelial ImmunoSPOT)分析进行分析通过各种来源的癌细胞释放全长CK19,并通过质谱分析CK19的序列。用环己酰亚胺,布雷菲德菌素A或长春新碱进行了其他功能性实验,以分析CK19释放的生物学特性。 CK19-EPISPOT用于检测45例乳腺癌患者的骨髓中已扩散的肿瘤细胞,然后对其进行平均6年的随访。结果CK19是通过结直肠癌(HT-29,HCT116,Caco-2)表达和释放的)和乳腺癌(MCF-7,SKBR3和MDA-MB-231)癌细胞系。 CK19-EPISPOT比CK19-ELISA更灵敏。带有针对不同CK19表位的抗体的双荧光EPISPOT显示了全长CK19的释放,这已通过质谱法确认。功能实验表明,CK19的释放是一个活跃的过程,而不仅仅是细胞死亡的结果。在44%至70%的乳腺癌患者的BM中可检测到CK19释放细胞(RCs)。 CK19-RCs的发生率和数量与明显转移相关,与没有这些细胞的患者相比,CK19-RCs的生存率降低(P = 0.025,对数秩检验; P = 0.0019,危险结论,全长CK19由活的上皮肿瘤细胞释放,并且CK19-RCs可能构成具有高转移特性的乳腺癌细胞的生物学活性子集。

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