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A platform of genetically engineered bacteria as vehicles for localized delivery of therapeutics: Toward applications for Crohns disease

机译:基因工程细菌作为平台用于局部递送治疗药物:克罗恩病的应用

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摘要

For therapies targeting diseases of the gastrointestinal tract, we and others envision probiotic bacteria that synthesize and excrete biotherapeutics at disease sites. Toward this goal, we have engineered commensal E. coli that selectively synthesize and secrete a model biotherapeutic in the presence of nitric oxide (NO), an intestinal biomarker for Crohn's disease (CD). This is accomplished by co‐expressing the pore forming protein TolAIII with the biologic, granulocyte macrophage‐colony stimulating factor (GM‐CSF). We have additionally engineered these bacteria to accumulate at sites of elevated NO by engineering their motility circuits and controlling pseudotaxis. Importantly, because we have focused on in vitro test beds, motility and biotherapeutics production are spatiotemporally characterized. Together, the targeted recognition, synthesis, and biomolecule delivery comprises a “smart” probiotics platform that may have utility in the treatment of CD. Further, this platform could be modified to accommodate other pursuits by swapping the promoter and therapeutic gene to reflect other disease biomarkers and treatments, respectively.
机译:对于针对胃肠道疾病的疗法,我们和其他人设想了在疾病部位合成和排泄生物疗法的益生菌。为了实现这一目标,我们设计了共生大肠杆菌,该大肠杆菌在存在一氧化氮(NO)(一种克罗恩氏病(CD)的肠道生物标志物)的情况下选择性合成和分泌一种生物治疗药物。这是通过将造孔蛋白TolAIII与生物性粒细胞巨噬细胞集落刺激因子(GM-CSF)共表达来实现的。我们还对这些细菌进行了工程改造,以通过设计其运动回路和控制伪趋向来在NO升高的部位积聚。重要的是,由于我们专注于体外试验床,因此可以在时间上对运动性和生物治疗药物的生产进行表征。靶向识别,合成和生物分子传递共同构成了一个“智能”益生菌平台,该平台可能在CD的治疗中具有实用性。此外,可以通过交换启动子和治疗基因以分别反映其他疾病生物标志物和治疗方法,对该平台进行修改以适应其他需求。

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