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. 2019 Dec;576(7787):452-458.
doi: 10.1038/s41586-019-1665-6. Epub 2019 Oct 23.

Chimeric peptidomimetic antibiotics against Gram-negative bacteria

Anatol Luther  1 Matthias Urfer  2 Michael Zahn  3 Maik Müller  4 Shuang-Yan Wang  2 Milon Mondal  2 Alessandra Vitale  5 Jean-Baptiste Hartmann  3 Timothy Sharpe  3 Fabio Lo Monte  2 Harsha Kocherla  2 Elizabeth Cline  2 Gabriella Pessi  5 Parthasarathi Rath  3 Seyed Majed Modaresi  3 Petra Chiquet  1 Sarah Stiegeler  1 Carolin Verbree  1 Tobias Remus  1 Michel Schmitt  1 Caroline Kolopp  1 Marie-Anne Westwood  1 Nicolas Desjonquères  1 Emile Brabet  1 Sophie Hell  1 Karen LePoupon  1 Annie Vermeulen  1 Régis Jaisson  1 Virginie Rithié  1 Grégory Upert  1 Alexander Lederer  1 Peter Zbinden  1 Achim Wach  1 Kerstin Moehle  2 Katja Zerbe  2 Hans H Locher  1 Francesca Bernardini  1 Glenn E Dale  1 Leo Eberl  5 Bernd Wollscheid  4 Sebastian Hiller  3 John A Robinson  6 Daniel Obrecht  7
Affiliations

Chimeric peptidomimetic antibiotics against Gram-negative bacteria

Anatol Luther et al. Nature. 2019 Dec.

Erratum in

  • Author Correction: Chimeric peptidomimetic antibiotics against Gram-negative bacteria.
    Luther A, Urfer M, Zahn M, Müller M, Wang SY, Mondal M, Vitale A, Hartmann JB, Sharpe T, Monte FL, Kocherla H, Cline E, Pessi G, Rath P, Modaresi SM, Chiquet P, Stiegeler S, Verbree C, Remus T, Schmitt M, Kolopp C, Westwood MA, Desjonquères N, Brabet E, Hell S, LePoupon K, Vermeulen A, Jaisson R, Rithié V, Upert G, Lederer A, Zbinden P, Wach A, Moehle K, Zerbe K, Locher HH, Bernardini F, Dale GE, Eberl L, Wollscheid B, Hiller S, Robinson JA, Obrecht D. Luther A, et al. Nature. 2019 Dec;576(7786):E5. doi: 10.1038/s41586-019-1810-2. Nature. 2019. PMID: 31758154

Abstract

There is an urgent need for new antibiotics against Gram-negative pathogens that are resistant to carbapenem and third-generation cephalosporins, against which antibiotics of last resort have lost most of their efficacy. Here we describe a class of synthetic antibiotics inspired by scaffolds derived from natural products. These chimeric antibiotics contain a β-hairpin peptide macrocycle linked to the macrocycle found in the polymyxin and colistin family of natural products. They are bactericidal and have a mechanism of action that involves binding to both lipopolysaccharide and the main component (BamA) of the β-barrel folding complex (BAM) that is required for the folding and insertion of β-barrel proteins into the outer membrane of Gram-negative bacteria. Extensively optimized derivatives show potent activity against multidrug-resistant pathogens, including all of the Gram-negative members of the ESKAPE pathogens1. These derivatives also show favourable drug properties and overcome colistin resistance, both in vitro and in vivo. The lead candidate is currently in preclinical toxicology studies that-if successful-will allow progress into clinical studies that have the potential to address life-threatening infections by the Gram-negative pathogens, and thus to resolve a considerable unmet medical need.

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References

    1. WHO. Global Priority List of Antibiotic-resistant Bacteria to Guide Research, Discovery, and Development of New Antibiotics (World Health Organization, Geneva, 2017).
    1. Boucher, H. W. et al. Bad bugs, no drugs: no ESKAPE! An update from the Infectious Diseases Society of America. Clin. Infect. Dis. 48, 1–12 (2009). - DOI
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    1. Henderson, J. C. et al. The power of asymmetry: architecture and assembly of the Gram-negative outer membrane bilayer. Annu. Rev. Microbiol. 70, 255–278 (2016). - DOI

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