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Liver metastatic model for human gastric cancer established by orthotopic tumor cell implantation.

机译:通过原位肿瘤细胞植入建立的人胃癌肝转移模型。

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摘要

We have established an orthotopic implantation model that is highly metastatic to the liver. A human gastric carcinoma cell line, AZ521, with low capacity for liver metastasis was implanted as a single-cell suspension in the stomach of nude mice. The tumor cells derived from a few liver metastatic foci were subsequently implanted orthotopically, and we established a cell line, AZH5G, by repeating the in vivo stepwise selection method. This metastasizing line (AZH5G) developed liver metastasis in seven of eight (87.5%) cases, whereas parental AZ521 developed in 3 of 20 (15.0%). The in vitro growth activities of AZH5G were lower than that of AZ521, although the in vivo tumorigenicity of AZH5G was clearly higher than that of AZ521. Motility assays demonstrated higher motility of AZH5G than of AZ521. Flow cytometric analysis demonstrated that the expression of alpha 6-integrin significantly decreased in AZH5G (4.9% +/- 4.1%) compared to in AZ521 (17.7% +/- 8.1%) (p < 0.05). The adhesive activity of AZH5G cells to laminin was lower than that of AZ521 cells. In contrast, the adhesive activity of AZH5G cells to fibronectin was clearly higher than that of AZ521 cells. These findings suggested that changes in the expression of integrins on the cell surface might play an important role in metastatic ability. This well characterized line and its in vivo experimental model should be useful to investigate the mechanisms of liver metastasis and to develop a new therapeutic approach for human gastric cancer.
机译:我们已经建立了对肝脏高度转移的原位植入模型。将具有低肝转移能力的人胃癌细胞系AZ521作为单细胞悬液植入裸鼠的胃中。随后原位植入源自几个肝脏转移灶的肿瘤细胞,并通过重复体内逐步选择方法,我们建立了AZH5G细胞系。该转移株(AZH5G)在八分​​之七(87.5%)的病例中发生了肝转移,而亲本AZ521在二十分之三的情况下(15.0%)发生了肝转移。尽管AZH5G的体内致瘤性明显高于AZ521,但AZH5G的体外生长活性低于AZ521。动力性分析表明,AZH5G的运动性高于AZ521。流式细胞仪分析显示,与AZ521(17.7%+/- 8.1%)相比,AZH5G(4.9%+/- 4.1%)中的α6-整合素表达显着降低(p <0.05)。 AZH5G细胞对层粘连蛋白的粘附活性低于AZ521细胞。相反,AZH5G细胞对纤连蛋白的粘附活性明显高于AZ521细胞。这些发现表明细胞表面整合素表达的改变可能在转移能力中起重要作用。此特征良好的系及其体内实验模型应有助于研究肝转移的机制并开发一种新的人胃癌治疗方法。

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