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细菌将一种新型细胞毒素递送至实体瘤缺氧区域。

Bacterial delivery of a novel cytolysin to hypoxic areas of solid tumors.

机构信息

Tumor Targeting Group, Academic Unit of Pathology, University of Sheffield Medical School, Sheffield, UK.

出版信息

Gene Ther. 2009 Mar;16(3):329-39. doi: 10.1038/gt.2008.188. Epub 2009 Jan 29.

Abstract

The efficacy of current anti-cancer gene therapies is limited by the inability of gene vectors to penetrate the poorly vascularized, hypoxic regions of tumors, leaving these sites untreated. We describe a new approach for targeting gene therapy to these sites, which employs an attenuated strain of the non-pathogenic bacterium, Salmonella typhimurium, carrying an exogenous (that is, reporter or therapeutic) gene under the regulation of a new, highly hypoxia-inducible promoter (FF+20()). This bacterial vector was seen to rapidly migrate into, and thrive in, hypoxic areas of both mammary tumor spheroids grown in vitro and orthotopic mammary tumors after systemic injection. Using the reporter gene construct, FF+20()-lacZ, we show that bacterial expression of high levels of beta-galactosidase occurred only in hypoxic/necrotic sites of spheroids and tumors. We then replaced the reporter gene with one encoding a novel cytotoxic protein (HlyE) and showed that this was also expressed by bacteria only in hypoxic regions of murine mammary tumors. This resulted in a marked increase in tumor necrosis and reduced tumor growth. Our system represents a promising new strategy for delivering gene therapy to poorly vascularized regions of tumors and shows, for the first time, the efficacy of HlyE as an anti-tumor agent.

摘要

当前的抗癌基因疗法的疗效受到限制,因为基因载体无法穿透肿瘤血管化不良、缺氧的区域,导致这些部位未得到治疗。我们描述了一种将基因治疗靶向这些部位的新方法,该方法使用减毒的非致病性细菌鼠伤寒沙门氏菌株,携带外源性(即报告基因或治疗基因),由一个新的、高度缺氧诱导的启动子(FF+20())调控。这种细菌载体被观察到能够快速迁移到体外培养的乳腺肿瘤球体和原位乳腺肿瘤的缺氧区域,并在其中茁壮成长。使用报告基因构建体 FF+20()-lacZ,我们表明,仅在球体和肿瘤的缺氧/坏死部位才会发生高水平的β-半乳糖苷酶的细菌表达。然后,我们用编码一种新型细胞毒性蛋白(HlyE)的基因取代报告基因,并表明该基因也仅在小鼠乳腺肿瘤的缺氧区域由细菌表达。这导致肿瘤坏死明显增加,肿瘤生长减少。我们的系统代表了向肿瘤血管化不良区域递送基因治疗的一种很有前途的新策略,并首次表明 HlyE 作为一种抗肿瘤剂的疗效。

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