首页> 外文期刊>Cancer gene therapy >Syn3 provides high levels of intravesical adenoviral-mediated gene transfer for gene therapy of genetically altered urothelium and superficial bladder cancer
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Syn3 provides high levels of intravesical adenoviral-mediated gene transfer for gene therapy of genetically altered urothelium and superficial bladder cancer

机译:Syn3可提供高水平的膀胱内腺病毒介导的基因转移,用于基因改变的尿路上皮和浅表性膀胱癌的基因治疗

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Using our model to grow superficial human bladder cancer in the mouse bladder, we have found that the polyamide compound, Syn3, when injected intravesically for 1 hour at 1 mg/mL on two consecutive days, markedly increases rAd-β-gal intravesical gene transfer and expression. This enhanced transgene expression was much greater than obtain by the use of 22% ethanol, which had previously been shown to increase intravesical adenoviral gene transfer, whereas little or no gene expression was seen with exposure to only rAd-β-gal. β-Galactosidase staining was seen in virtually every normal urothelial and superficial tumor cell present, including tumors that express little or no coxsackie–adenovirus receptors when Syn3 was present. High adenoviral-mediated gene transfer was also documented in the pig bladder using Syn3 in a similar protocol. Therefore, Syn3 may overcome the limitations of adequate intravesical adenoviral-mediated gene transfer and, when combined with an appropriate adenoviral-mediated gene, could offer an effective approach to the treatment of superficial bladder cancer and perhaps even genetically altered precursor lesions.
机译:使用我们的模型在小鼠膀胱中生长浅表性人膀胱癌,我们发现聚酰胺化合物Syn3在连续两天以1 mg / mL膀胱内注射1小时后,可明显增加rAd-β-gal膀胱内基因的转移和表达。这种增强的转基因表达远大于使用22%乙醇获得的转基因表达,后者先前已显示出可增加膀胱内腺病毒基因转移,而仅暴露于rAd-β-gal则几乎看不到基因表达。几乎在所有正常的尿路上皮和浅表肿瘤细胞中都可见到β-半乳糖苷酶染色,包括当存在Syn3时表达很少或没有柯萨奇腺病毒受体的肿瘤。在类似方案中,还使用Syn3在猪膀胱中记录了高腺病毒介导的基因转移。因此,Syn3可以克服腺泡病毒介导的基因转移的局限性,当与适当的腺病毒介导的基因结合使用时,可以为浅表性膀胱癌甚至基因改变的前体病变提供有效的治疗方法。

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