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通过工程手段生产并分泌大肠杆菌素以实现对生物膜细胞的快速选择性杀伤。

Engineering to produce and secrete colicins for rapid and selective biofilm cell killing.

作者信息

Jin Xing, An Sungjun, Kightlinger Weston, Zhou Jiacheng, Hong Seok Hoon

机构信息

Department of Chemical and Biological Engineering, Illinois Institute of Technology, Chicago, IL 60616, USA.

Department of Chemical and Biological Engineering, Northwestern University, Evanston, IL 60208, USA.

出版信息

AIChE J. 2021 Dec;67(12). doi: 10.1002/aic.17466. Epub 2021 Sep 23.

Abstract

Bacterial biofilms are associated with chronic infectious diseases and are highly resistant to conventional antibiotics. Antimicrobial bacteriocins are alternatives to conventional antibiotics and are characterized by unique cell-killing mechanisms, including pore formation on cell membranes, nuclease activity, and cell wall synthesis inhibition. Here, we used cell-free protein synthesis to rapidly evaluate the anti-biofilm activities of colicins E1, E2, and E3. We found that E2 (with DNase activity) most effectively killed target biofilm cells (., the K361 strain) while leaving non-targeted biofilms intact. We then engineered probiotic microorganisms with genetic circuits to controllably synthesize and secrete colicin E2, which successfully inhibited biofilms and killed pre-formed indicator biofilms. Our findings suggest that colicins rapidly and selectively kill target biofilm cells in multispecies biofilms and demonstrate the potential of using microorganisms engineered to produce antimicrobial colicin proteins as live therapeutic strategies to treat biofilm-associated infections.

摘要

细菌生物膜与慢性传染病相关,并且对传统抗生素具有高度抗性。抗菌细菌素是传统抗生素的替代品,其特点是具有独特的细胞杀伤机制,包括在细胞膜上形成孔道、核酸酶活性以及抑制细胞壁合成。在这里,我们使用无细胞蛋白质合成来快速评估大肠杆菌素E1、E2和E3的抗生物膜活性。我们发现E2(具有DNA酶活性)最有效地杀死了目标生物膜细胞(即K361菌株),同时使非目标生物膜保持完整。然后,我们利用基因电路对益生菌进行工程改造,以可控地合成和分泌大肠杆菌素E2,其成功抑制了生物膜并杀死了预先形成的指示生物膜。我们的研究结果表明,大肠杆菌素能快速、选择性地杀死多物种生物膜中的目标生物膜细胞,并证明了利用经过工程改造以产生抗菌大肠杆菌素蛋白的微生物作为治疗生物膜相关感染的活疗法的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b190/10015990/508c9e3075e4/AIC-67-0-g004.jpg

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