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首页> 外文期刊>Molecular & cellular proteomics: MCP >Proteomic screening of anaerobically regulated promoters from Salmonella and its antitumor applications.
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Proteomic screening of anaerobically regulated promoters from Salmonella and its antitumor applications.

机译:沙门氏菌厌氧调控启动子的蛋白质组学筛选及其抗肿瘤应用。

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摘要

Solid tumors often contain hypoxic and necrotic areas that can be targeted by attenuated Salmonella typhimurium VNP20009 (VNP). We sought to develop a hypoxia- inducible promoter system based on the tumor-specific delivered strain VNP to confine expression of therapeutic gene specifically or selectively within the tumor microenvironment. A hypoxia-inducible promoter - adhE promoter was screened from the hypoxia-regulated endogenous proteins of Salmonella through two-dimensional gel electrophoresis and matrix-assisted laser desorption ionization-time-of-flight/time-of-flight MS-based proteomics approaches. The efficiency and specificity of the selected adhE promoter were validated first in both bacteria and animal tumor models. The adhE promoter could specifically drive GFP gene expression under hypoxia, but not under normoxia. Furthermore, luciferase reporter expression controlled by the system was also confined to the tumors. Finally, we investigated the anticancer efficacy of VNP delivering human endostatin controlled by our adhE promoter system in both murine melanoma and Lewis lung carcinoma models. Our results demonstrated that by the dual effects of tumoricidal and anti-angiogenic activities, the recombinant Salmonella strain could generate enhanced antitumor effects compared with those of unarmed VNP treatment or untreated control. The recombinant VNP could retard tumor growth significantly and extend survival of tumor-bearing mice by inducing more apoptosis and more severe necrosis as well as inhibiting blood vessel density within tumors. Therefore, VNP carrying the endostatin gene under our tumor-targeted expression system holds promise for the treatment of solid tumors.
机译:实体瘤通常包含缺氧和坏死区域,减毒鼠伤寒沙门氏菌VNP20009(VNP)可以靶向这些区域。我们试图开发一种基于肿瘤特异性递送菌株VNP的低氧诱导型启动子系统,以在肿瘤微环境中特异性或选择性地限制治疗基因的表达。通过二维凝胶电泳和基质辅助激光解吸电离飞行时间/飞行时间MS蛋白质组学方法,从低氧调节的沙门氏菌内源蛋白中筛选出了一个缺氧诱导型启动子-adhE启动子。首先在细菌和动物肿瘤模型中都验证了所选的adhE启动子的效率和特异性。在缺氧条件下,adhE启动子可以特异性驱动GFP基因的表达,而在常氧条件下则不能。此外,受系统控制的荧光素酶报道基因的表达也仅限于肿瘤。最后,我们在鼠黑素瘤和Lewis肺癌模型中研究了由adhE启动子系统控制的VNP递送人内皮抑素的抗癌功效。我们的结果表明,与无武装的VNP处理或未经处理的对照相比,重组沙门氏菌菌株通过具有杀伤性和抗血管生成活性的双重作用,可以产生增强的抗肿瘤作用。重组VNP通过诱导更多的细胞凋亡和更严重的坏死以及抑制肿瘤内的血管密度,可以显着延迟肿瘤的生长并延长荷瘤小鼠的生存期。因此,在我们的肿瘤靶向表达系统下携带内皮抑素基因的VNP有望用于实体瘤的治疗。

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