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首页> 外文期刊>Experimental dermatology >Evaluation of combined gene regulatory elements for transcriptional targeting of suicide gene expression to malignant melanoma.
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Evaluation of combined gene regulatory elements for transcriptional targeting of suicide gene expression to malignant melanoma.

机译:评估自杀基因表达转录靶向恶性黑色素瘤的基因调控元件。

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摘要

Selective killing of tumors can be achieved by targeting the transcription of suicide genes via specific DNA control elements to malignant cells. Three different enhancer-promoter systems were constructed and evaluated for their capability to direct gene expression to melanoma. Two tissue-specific (tyrosine and MIA) promoters and one weak viral promoter were fused to multiple tandem copies of a melanocyte-specific enhancer element. Reporter gene assays revealed a maximum increase in transcription by combining each promoter with 3-4 copies of the enhancer and demonstrated that all enhancer-promoter combinations exhibited tissue-specific activity. Though this activity was still significantly less than that of the strong but unspecific cytomegalovirus (CMV) promoter. In contrast, when those combinations were employed to drive the expression of two suicide genes, encoding the diptheria toxin A chain (DT-A) and the prodrug-activating herpes simplex virus thymidine kinase (TK), respectively, only those constructs in which transcription was under control of tissue-specific promoter elements mediated selective killing of melanoma cells. This killing was in the range of cell death induced by CMV promoter activity. Our data indicate that the enhancer/tyrosinase and enhancer/MIA promoter constructs but not the viral promoter constructs can provide a valuable tool for selective suicide gene expression in melanoma.
机译:可以通过将自杀基因的转录通过特定的DNA控制元件靶向恶性细胞来实现对肿瘤的选择性杀伤。构建了三种不同的增强子-启动子系统,并评估了它们将基因表达导向黑素瘤的能力。将两个组织特异性(酪氨酸和MIA)启动子和一个弱病毒启动子与黑色素细胞特异性增强子元件的多个串联拷贝融合。记者基因检测揭示了通过将每个启动子与3-4个拷贝的增强子结合在一起,转录的最大增加,并证明所有增强子-启动子组合均表现出组织特异性活性。尽管此活性仍显着低于强但非特异性巨细胞病毒(CMV)启动子的活性。相反,当采用这些组合来驱动两个自杀基因的表达时,分别编码白喉毒素A链(DT-A)和激活前药的单纯疱疹病毒胸苷激酶(TK),只有那些转录在组织特异性启动子元件介导的黑色素瘤细胞选择性杀伤的控制下。该杀伤在CMV启动子活性诱导的细胞死亡范围内。我们的数据表明,增强子/酪氨酸酶和增强子/ MIA启动子构建体而非病毒启动子构建体可以为黑色素瘤中选择性自杀基因表达提供有价值的工具。

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