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Transcriptional targeting of tumors with a novel tumor-specific survivin promoter

机译:新型肿瘤特异性survivin启动子的转录靶定

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It has been demonstrated that survivin, a novel member of the inhibitor of apoptosis (IAP) protein family, is expressed in human cancers but is undetectable in normal differentiated tissues. We employed a recombinant adenoviral vector (reAdGL3BSurvivin) in which a tumor-specific survivin promoter and a luciferase reporter gene were inserted into the E1-deleted region of adenovirus vector. Luciferase activity was measured in both multiple tumor cell lines and two primary melanoma cells infected with reAdGL3BSurvivin. Human fibroblast and mammary epithelial cell lines were used as negative controls. A reAdGL3CMV, containing the CMV promoter and luciferase gene, was used as a positive control to normalize the luciferase activity generated by the survivin promoter. Our data revealed that the survivin promoter showed high activity in both established tumor cell lines and the primary melanoma cells. In contrast, the in vivo studies indicated that the activities of survivin promoter were extremely low in the major mouse organs. The survivin promoter appears to be a promising tumor-specific promoter exhibiting a "tumor on" and "liver off" profile, and therefore, it may prove to be a good candidate for transcriptional targeting of cancer gene therapy in a wide variety of tumors.
机译:已经证明,survivin是细胞凋亡抑制剂(IAP)蛋白家族的新成员,在人类癌症中表达,但在正常分化的组织中未检测到。我们采用了重组腺病毒载体(reAdGL3BSurvivin),其中将肿瘤特异性survivin启动子和荧光素酶报道基因插入了腺病毒载体的E1缺失区域。在被reAdGL3BSurvivin感染的多个肿瘤细胞系和两个原发性黑色素瘤细胞中都测量了萤光素酶活性。人成纤维细胞和乳腺上皮细胞系用作阴性对照。包含CMV启动子和萤光素酶基因的reAdGL3CMV被用作阳性对照,以正常化由survivin启动子产生的萤光素酶活性。我们的数据显示,survivin启动子在已建立的肿瘤细胞系和原发性黑色素瘤细胞中均显示出高活性。相反,体内研究表明,survivin启动子的活性在主要小鼠器官中极低。 survivin启动子似乎是一种有前途的肿瘤特异性启动子,表现出“肿瘤开启”和“脱离”状态,因此,它可能被证明是在多种肿瘤中靶向靶向癌基因治疗的良好候选者。

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