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CanScript an 18-Base pair DNA sequence boosts tumor cell-specific promoter activity

机译:CanScript是一个18个碱基对的DNA序列可增强肿瘤细胞特异性启动子的活性

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摘要

Gene therapy protocols for the treatment of cancer often employ gene promoter sequences that are known to be overexpressed in specific tumor cell types relative to normal cells. These promoters, while specific, are often weakly active. It would be desirable to increase the activity of such promoters, while at the same time retain specificity, so that the therapeutic gene is more robustly expressed. Using a luciferase reporter DNA construct in both in vitro cell transfection assays and in vivo mouse tumor models, we have determined that in the absence of any other DNA sequence, a previously identified 18-base pair enhancer sequence called CanScript, lying upstream of the MSLN gene, has ∼25% of the promoter activity of CAG, a very strong non-specific promoter/enhancer, in tumor cells in which MSLN is highly expressed. Furthermore, tandem repeat copies of CanScript enhance transcription in a dose-dependent manner and, when coupled with promoter sequences that are active in tumor cells, increase promoter activity. These findings suggest that the incorporation of CanScript into gene constructs may have application in enhancing activity of promoters used in cancer-targeting gene therapy strategies, thereby improving therapeutic efficacy.
机译:用于治疗癌症的基因治疗方案通常采用已知在特定肿瘤细胞类型中相对于正常细胞过表达的基因启动子序列。这些启动子虽然是特异性的,但通常活性很弱。期望增加此类启动子的活性,同时保留特异性,从而使治疗基因更稳定地表达。在体外细胞转染测定和体内小鼠肿瘤模型中使用荧光素酶报道基因DNA构建体,我们已经确定,在不存在任何其他DNA序列的情况下,先前鉴定出的18碱基对增强子序列CanScript位于MSLN的上游该基因在MSLN高度表达的肿瘤细胞中,具有约25%的CAG启动子活性,CAG是一种非常强的非特异性启动子/增强子。此外,CanScript的串联重复拷贝以剂量依赖性方式增强转录,并且当与在肿瘤细胞中有活性的启动子序列偶联时,会增加启动子活性。这些发现表明,将CanScript并入基因构建体中可用于增强靶向癌症的基因治疗策略中使用的启动子的活性,从而提高治疗效果。

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