<p>Precision antimicrobials that can kill pathogens without damaging host commensals hold potential to cure disease without antibiotic-associated dysbiosis. Here we report the <i>de novo</i> design of host defense peptides that have been rationally engineered to precisely target specific pathogens by mimicking key molecular features of the target microbe’s unique channel-forming membrane proteins, or porins. This biomimetic strategy exploits physical and structural motifs of the pathogen envelope, rather than targeting resistance-susceptible protein biochemical pathways, to construct fast-acting precision bacteriolytics. Utilizing this approach, we design an antitubercular sequence that undergoes instructed, tryptophan-zippered assembly within the mycolic-acid rich outer membrane of <i>Mycobacterium tuberculosis</i> (Mtb) to specifically kill the pathogen without collateral toxicity towards lung commensals or host tissue. These mycomembrane-templated mechanisms are rapid and synergistically enhance the potency of antibiotics that otherwise poorly diffuse across the rigid Mtb envelope, particularly those that exploit porins for antimycobacterial activity. This new porin-mimetic paradigm may serve as a conceptual basis for the directed design of new narrow-spectrum antimicrobial scaffolds.</p>
<p>Precision antimicrobials that can kill pathogens without damaging host commensals hold potential to cure disease without antibiotic-associated dysbiosis. Here we report the <i>de novo</i> design of host defense peptides that have been rationally engineered to precisely target specific pathogens by mimicking key molecular features of the target microbe’s unique channel-forming membrane proteins, or porins. This biomimetic strategy exploits physical and structural motifs of the pathogen envelope, rather than targeting resistance-susceptible protein biochemical pathways, to construct fast-acting precision bacteriolytics. Utilizing this approach, we design an antitubercular sequence that undergoes instructed, tryptophan-zippered assembly within the mycolic-acid rich outer membrane of <i>Mycobacterium tuberculosis</i> (Mtb) to specifically kill the pathogen without collateral toxicity towards lung commensals or host tissue. These mycomembrane-templated mechanisms are rapid and synergistically enhance the potency of antibiotics that otherwise poorly diffuse across the rigid Mtb envelope, particularly those that exploit porins for antimycobacterial activity. This new porin-mimetic paradigm may serve as a conceptual basis for the directed design of new narrow-spectrum antimicrobial scaffolds.</p>
scite is a Brooklyn-based organization that helps researchers better discover and understand research articles through Smart Citations–citations that display the context of the citation and describe whether the article provides supporting or contrasting evidence. scite is used by students and researchers from around the world and is funded in part by the National Science Foundation and the National Institute on Drug Abuse of the National Institutes of Health.
hi@scite.ai
10624 S. Eastern Ave., Ste. A-614
Henderson, NV 89052, USA
Copyright © 2024 scite LLC. All rights reserved.
Made with 💙 for researchers
Part of the Research Solutions Family.