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首页> 外文期刊>International Journal of Clinical and Experimental Medicine >Development of targeted therapy for a broad spectrum of solid tumors mediated by a double promoter plasmid expressing diphtheria toxin under the control of IGF2-P4 and IGF2-P3 regulatory sequences
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Development of targeted therapy for a broad spectrum of solid tumors mediated by a double promoter plasmid expressing diphtheria toxin under the control of IGF2-P4 and IGF2-P3 regulatory sequences

机译:在IGF2-P4和IGF2-P3调控序列的控制下,针对表达白喉毒素的双启动子质粒介导的广泛实体瘤靶向治疗的开发

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摘要

Background: The human IGF2-P4 and IGF2-P3 promoters are highly active in a variety of human cancers, while existing at a nearly undetectable level in the surrounding normal tissue. Thus, a double promoter DTA-expressing vector was created, carrying on a single construct two separate genes expressing the diphtheria toxin a-fragment (DTA), from two different regulatory sequences, selected from the cancer-specific promoters IGF2-P4 and IGF2-P3. Methods: The therapeutic potential of the double promoter toxin vector P4-DTA-P3-DTA was tested in different cancer cells (pancreatic cancer, ovarian cancer and HCC). Results: The double promoter vector P4-DTA-P3-DTA exhibited superior inhibition activity in different cancer cell lines, compared to the single promoter expression vectors activity. Conclusions: Our findings suggest that administration of P4-DTA-P3-DTA has the potential to reach and eradicate tumor cells and thus may help reduce tumor burden, improve the quality of life of the patients; and prolong their life span.
机译:背景:人类IGF2-P4和IGF2-P3启动子在多种人类癌症中具有很高的活性,而在周围正常组织中却以几乎不可检测的水平存在。因此,创建了表达双启动子的DTA的载体,其在单个构建体上携带两个不同的表达白喉毒素α片段(DTA)的独立基因,其选自两个不同的调控序列,所述调控序列选自癌症特异性启动子IGF2-P4和IGF2- P3。方法:在不同的癌细胞(胰腺癌,卵巢癌和HCC)中测试了双启动子毒素载体P4-DTA-P3-DTA的治疗潜力。结果:与单启动子表达载体活性相比,双启动子载体P4-DTA-P3-DTA在不同癌细胞系中表现出优异的抑制活性。结论:我们的研究结果表明,P4-DTA-P3-DTA的给药有可能到达和根除肿瘤细胞,因此可能有助于减轻肿瘤负担,改善患者的生活质量;并延长他们的寿命。

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