首页> 外文期刊>The Journal of Urology >Use of an anti-ras ribozyme to alter the malignant phenotype of a human bladder cancer cell line.
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Use of an anti-ras ribozyme to alter the malignant phenotype of a human bladder cancer cell line.

机译:抗ras核酶改变人膀胱癌细胞系恶性表型的用途。

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PURPOSE: In this study, we evaluated the ability of a ribozyme (catalytic RNA), which site specifically cleaves the mRNA of the activated H-ras gene, to alter the malignant phenotype of an invasive human bladder cancer cell line. MATERIALS AND METHODS: The human bladder cancer cell line EJ which contains the activated H-ras gene was used in these studies. Cell lines with and without the anti-ras ribozyme were examined for their malignant potential in athymic (nude) mice by using an orthotopic model of bladder cancer. Endpoints evaluated included tumor take and animal survival. RESULTS: EJ tumors containing the anti-ras ribozyme showed a reduction in tumor take (35% versus 45%) and prolonged survival (74 days versus 65 days) compared with standard EJ cells. This survival advantage was not as pronounced as anticipated. To evaluate this finding, we examined the tumor from mice originally inoculated with the ribozyme-containing cell line to determine if the ribozyme was still present. Approximately 60% of the animals had lost ribozyme expression. Animals that maintained ribozyme expression had a mean survival of 81 +/- 4 days which was significantly prolonged compared with control mice (65 +/- 5 days). CONCLUSION: This study suggests that the invasive phenotype is blunted with the anti-ras ribozyme, delaying but not abolishing the metastatic phenotype. These results further delineate the roles of ras genes in malignancy and demonstrate that ribozymes may be a powerful tool for exploring the role of individual oncogenes and may be used as anticancer agents.
机译:目的:在这项研究中,我们评估了一个核酶(催化RNA)的能力,该酶特异性地切割活化的H-ras基因的mRNA,以改变侵袭性人膀胱癌细胞系的恶性表型。材料与方法:在这些研究中使用了包含激活的H-ras基因的人膀胱癌细胞系EJ。通过使用膀胱癌的原位模型,检查了有无抗ras核酶的细胞系在无胸腺(裸)小鼠中的恶性潜能。评估的终点包括肿瘤摄取和动物存活。结果:与标准EJ细胞相比,含有抗ras核酶的EJ肿瘤的肿瘤摄取减少(35%对45%),并延长了生存期(74天对65天)。这种生存优势并不像预期的那么明显。为了评估这一发现,我们检查了最初接种含核酶细胞系的小鼠的肿瘤,以确定是否仍然存在核酶。大约60%的动物失去了核酶表达。维持核酶表达的动物的平均生存期为81 +/- 4天,与对照小鼠(65 +/- 5天)相比,显着延长。结论:这项研究表明,抗ras核酶使浸润性表型变钝,延迟但不消除转移表型。这些结果进一步描述了ras基因在恶性肿瘤中的作用,并证明核酶可能是探索单个癌基因作用的有力工具,并可用作抗癌药。

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