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Targeting of adenovirus to human renal cell carcinoma cells.

机译:腺病毒靶向人肾细胞癌细胞。

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OBJECTIVES: The use of recombinant adenoviruses in cancer gene therapy is limited by the widespread expression of the coxsackievirus and adenovirus receptor on normal human cells. Targeting adenoviral vectors to renal cell carcinoma (RCC) cells may improve their potential in cancer gene therapy of patients with metastatic RCC. The G250 protein, also known as the carbonic anhydrase IX protein, is membranously expressed in all cases of clear cell RCC, and clinical studies have demonstrated exceptional tumor targeting with a G250 monoclonal antibody. METHODS: A recombinant bispecific single-chain antibody directed against the RCC-associated G250 protein and the adenovirus fiber knob domain was constructed and used to retarget recombinant adenovirus expressing the green fluorescent protein under control of the cytomegalovirus promoter. G250-specific adenoviral transduction of cells was examined by flow cytometric analysis of green fluorescent protein expression. RESULTS: G250-positive RCC cells displayed enhanced susceptibility for transduction by the green fluorescent protein recombinant adenovirus complexed with the G250-directed bispecific single-chain antibody when compared with native adenovirus. This enhanced transduction was restricted to G250-positive RCC cells and could be abolished completely in the presence of excess G250 protein. CONCLUSIONS: The results of this study demonstrate the feasibility of immunologic retargeting of adenovirus to RCC cells with the highly tumor-specific G250 protein as the target. This strategy may provide the possibility of improving cancer gene therapy for patients with RCC.
机译:目的:重组腺病毒在癌症基因治疗中的应用受到柯萨奇病毒和腺病毒受体在正常人细胞上的广泛表达的限制。将腺病毒载体靶向肾细胞癌(RCC)细胞可能会提高其在转移性RCC患者癌症基因治疗中的潜力。 G250蛋白,也称为碳酸酐酶IX蛋白,在所有透明细胞RCC的情况下均会膜状表达,并且临床研究表明,使用G250单克隆抗体可实现出色的肿瘤靶向性。方法:构建针对RCC相关G250蛋白和腺病毒纤维结结构域的重组双特异性单链抗体,并在巨细胞病毒启动子的控制下,将表达绿色荧光蛋白的重组腺病毒重新靶向。通过绿色荧光蛋白表达的流式细胞术分析检查细胞的G250特异性腺病毒转导。结果:与天然腺病毒相比,G250阳性RCC细胞显示出绿色荧光蛋白重组腺病毒与G250定向双特异性单链抗体复合的转导敏感性。这种增强的转导作用仅限于G250阳性RCC细胞,在过量的G250蛋白存在下可以完全消除。结论:这项研究的结果证明了以高度肿瘤特异性G250蛋白为靶标的腺病毒对RCC细胞进行免疫学重新靶向的可行性。这种策略可能为改善RCC患者的癌症基因治疗提供可能性。

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