Engineering to Produce and Secrete Colicins for Rapid and Selective Biofilm Cell Killing

Overview

Journal AIChE J

Date 2022 Nov 4

PMID 36329688

Authors

Xing Jin

Sungjun An

Weston Kightlinger

Jiacheng Zhou

Seok Hoon Hong

Affiliations

Soon will be listed here.

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.

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