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工程噬菌体靶向基因网络作为抗生素治疗的佐剂

Engineered bacteriophage targeting gene networks as adjuvants for antibiotic therapy.

作者信息

Lu Timothy K, Collins James J

机构信息

Harvard-Massachusetts Institute of Technology Division of Health Sciences and Technology, Cambridge, MA 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 2009 Mar 24;106(12):4629-34. doi: 10.1073/pnas.0800442106. Epub 2009 Mar 2.

Abstract

Antimicrobial drug development is increasingly lagging behind the evolution of antibiotic resistance, and as a result, there is a pressing need for new antibacterial therapies that can be readily designed and implemented. In this work, we engineered bacteriophage to overexpress proteins and attack gene networks that are not directly targeted by antibiotics. We show that suppressing the SOS network in Escherichia coli with engineered bacteriophage enhances killing by quinolones by several orders of magnitude in vitro and significantly increases survival of infected mice in vivo. In addition, we demonstrate that engineered bacteriophage can enhance the killing of antibiotic-resistant bacteria, persister cells, and biofilm cells, reduce the number of antibiotic-resistant bacteria that arise from an antibiotic-treated population, and act as a strong adjuvant for other bactericidal antibiotics (e.g., aminoglycosides and beta-lactams). Furthermore, we show that engineering bacteriophage to target non-SOS gene networks and to overexpress multiple factors also can produce effective antibiotic adjuvants. This work establishes a synthetic biology platform for the rapid translation and integration of identified targets into effective antibiotic adjuvants.

摘要

抗菌药物的研发越来越落后于抗生素耐药性的演变,因此,迫切需要能够轻松设计和实施的新型抗菌疗法。在这项研究中,我们对噬菌体进行工程改造,使其过量表达蛋白质并攻击抗生素未直接靶向的基因网络。我们发现,用工程噬菌体抑制大肠杆菌中的SOS网络,可在体外将喹诺酮类药物的杀菌效果提高几个数量级,并显著提高感染小鼠在体内的存活率。此外,我们证明工程噬菌体可以增强对耐药菌、持留菌和生物膜菌的杀伤作用,减少抗生素处理群体中产生的耐药菌数量,并作为其他杀菌抗生素(如氨基糖苷类和β-内酰胺类)的强效佐剂。此外,我们还表明,对噬菌体进行工程改造以靶向非SOS基因网络并过量表达多种因子,也可以产生有效的抗生素佐剂。这项工作建立了一个合成生物学平台,用于将已确定的靶点快速转化并整合为有效的抗生素佐剂。

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