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Proteasenexpression einzelner disseminierter Tumorzellen aus Lymphknoten und Knochenmark von Patienten mit nichtkleinzelligem Bronchialkarzinom

机译:非小细胞肺癌患者淋巴结和骨髓中单个播散性肿瘤细胞的蛋白酶表达

摘要

Non-small cell lung cancer (NSCLC) is characterised by early dissemination of tumor cells resulting in a strikingly reduced overall survival despite complete surgical removal of the primary tumour. It has been suggested that proteases contribute to this apparent aggressiveness of lung cancer because they are involved in a variety of mechanisms associated with tumor progression such as invasion, migration and angiogenesis. To investigate the significance of protease expression and to identify potentially co-regulated molecules during early dissemination and in minimal residual disease, we performed cDNA array analysis of single disseminated cancer cells or small cell clusters isolated from bone marrow and lymph nodes of NSCLC patients. We obtained macroscopically tumor free lymph nodes and bone marrow aspirates from patients with operable NSCLC and enriched single disseminated cancer cells and small cell clusters by density gradient centrifugation. Subsequently, the freshly prepared cell suspensions were stained with an antibody against the epithelial surface molecule EpCAM and single positive tumour cells were isolated by micromanipulation. After global amplification of the single cell cDNA and non-radioactive labelling proteinase expression was assessed using a cDNA array consisting of several matrix metalloproteases, cathepsins, caspases, kallikreins and other serine / cysteine proteases. Until now we could isolate 46 EpCAM+ cells from 72 lymph nodes and 19 EpCAM+ cells from 71 bone marrow aspirates. For 30 cells the epithelial origin could be confirmed by the co-expression of several epithelial markers or by expression of the tumor specific MAGE antigens. Hybridisation of these cells on our protease cDNA array revealed the expression of various proteases in single cells and small cell clusters. Particularly, serine proteases, cathepsins and other cysteine proteinases are frequently expressed, while, contrary to our expectations, the transcripts of matrix metalloproteases (MMP) were rarely detected in the analysed cells.
机译:非小细胞肺癌(NSCLC)的特征是尽早扩散肿瘤细胞,尽管手术切除了原发肿瘤,但总生存期却明显降低。已经表明蛋白酶有助于这种明显的肺癌侵袭性,因为蛋白酶参与了与肿瘤进展相关的多种机制,例如侵袭,迁移和血管生成。为了研究蛋白酶表达的重要性,并在早期传播和最小残留疾病中鉴定潜在的共调节分子,我们对从NSCLC患者的骨髓和淋巴结分离出的单个弥散性癌细胞或小细胞簇进行了cDNA阵列分析。我们从可手术的NSCLC患者中获得了无肿瘤的淋巴结和骨髓抽吸物,并通过密度梯度离心法富集了单个扩散的癌细胞和小细胞簇。随后,将新鲜制备的细胞悬液用抗上皮表面分子EpCAM的抗体染色,并通过显微操作分离单个阳性肿瘤细胞。整体扩增单细胞cDNA和非放射性标记蛋白酶后,使用由几种基质金属蛋白酶,组织蛋白酶,胱天蛋白酶,激肽释放酶和其他丝氨酸/半胱氨酸蛋白酶组成的cDNA阵列评估蛋白酶的表达。到目前为止,我们可以从72个淋巴结中分离出46个EpCAM +细胞,并从71个骨髓穿刺物中分离出19个EpCAM +细胞。对于30个细胞,上皮起源可以通过几种上皮标志物的共表达或通过肿瘤特异性MAGE抗原的表达来确认。这些细胞在我们的蛋白酶cDNA阵列上的杂交揭示了各种蛋白酶在单细胞和小细胞簇中的表达。特别是,经常表达丝氨酸蛋白酶,组织蛋白酶和其他半胱氨酸蛋白酶,而与我们的预期相反,在分析的细胞中很少检测到基质金属蛋白酶(MMP)的转录本。

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  • 作者

    Schilling Sabine;

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  • 年度 2005
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  • 原文格式 PDF
  • 正文语种 {"code":"de","name":"German","id":7}
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