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首页> 外文期刊>Cancer Cell International >Cell fusion in tumor progression: the isolation of cell fusion products by physical methods
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Cell fusion in tumor progression: the isolation of cell fusion products by physical methods

机译:肿瘤进展中的细胞融合:通过物理方法分离细胞融合产物

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摘要

Cell fusion induced by polyethylene glycol (PEG) is an efficient but poorly controlled procedure for obtaining somatic cell hybrids used in gene mapping, monoclonal antibody production, and tumour immunotherapy. Genetic selection techniques and fluorescent cell sorting are usually employed to isolate cell fusion products, but both procedures have several drawbacks. Here we describe a simple improvement in PEG-mediated cell fusion that was obtained by modifying the standard single-step procedure. We found that the use of two PEG undertreatments obtains a better yield of cell fusion products than the standard method, and most of these products are bi- or trinucleated polykaryocytes. Fusion rate was quantified using fluorescent cell staining microscopy. We used this improved cell fusion and cell isolation method to compare giant cells obtained in vitro and giant cells obtained in vivo from patients with Hodgkin's disease and erythroleukemia. In the present study we show how to improve PEG-mediated cell fusion and that cell separation by velocity sedimentation offers a simple alternative for the efficient purification of cell fusion products and to investigate giant cell formation in tumor development.
机译:聚乙二醇(PEG)诱导的细胞融合是一种有效的但控制不佳的程序,用于获得用于基因定位,单克隆抗体生产和肿瘤免疫疗法的体细胞杂种。通常采用遗传选择技术和荧光细胞分选方法来分离细胞融合产物,但是这两种方法都有一些缺点。在这里,我们描述了通过修改标准单步程序获得的PEG介导的细胞融合的简单改善。我们发现使用两种PEG不足处理可获得比标准方法更好的细胞融合产物产量,并且这些产物大多数是双核或三核多核细胞。使用荧光细胞染色显微镜定量融合率。我们使用这种改进的细胞融合和细胞分离方法来比较霍奇金病和红白血病患者体外获得的巨细胞和体内获得的巨细胞。在本研究中,我们展示了如何改善PEG介导的细胞融合,以及通过速度沉降进行的细胞分离为有效纯化细胞融合产物和研究肿瘤发展中巨细胞形成提供了简单的选择。

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