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De novo design and in vivo activity of conformationally restrained antimicrobial arylamide foldamers.


ABSTRACT: The emergence of drug-resistant bacteria has compromised the use of many conventional antibiotics, leading to heightened interest in a variety of antimicrobial peptides. Although these peptides have attractive potential as antibiotics, their size, stability, tissue distribution, and toxicity have hampered attempts to harness these capabilities. To address such issues, we have developed small (molecular mass <1,000 Da) arylamide foldamers that mimic antimicrobial peptides. Hydrogen-bonded restraints in the arylamide template rigidify the conformation via hydrogen bond formation and increase activity toward Staphylococcus aureus and Escherichia coli. The designed foldamers are highly active against S. aureus in an animal model. These results demonstrate the application of foldamer templates as therapeutics.

SUBMITTER: Choi S 

PROVIDER: S-EPMC2667368 | biostudies-literature | 2009 Apr

REPOSITORIES: biostudies-literature

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De novo design and in vivo activity of conformationally restrained antimicrobial arylamide foldamers.

Choi Sungwook S   Isaacs Andre A   Clements Dylan D   Liu Dahui D   Kim Hyemin H   Scott Richard W RW   Winkler Jeffrey D JD   DeGrado William F WF  

Proceedings of the National Academy of Sciences of the United States of America 20090409 17


The emergence of drug-resistant bacteria has compromised the use of many conventional antibiotics, leading to heightened interest in a variety of antimicrobial peptides. Although these peptides have attractive potential as antibiotics, their size, stability, tissue distribution, and toxicity have hampered attempts to harness these capabilities. To address such issues, we have developed small (molecular mass <1,000 Da) arylamide foldamers that mimic antimicrobial peptides. Hydrogen-bonded restrai  ...[more]

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