Controlling resistant bacteria with a novel class of β-lactamase inhibitor peptides: from rational design to in vivo analyses

Mandal, Santi M. ; Migliolo, Ludovico ; Silva, Osmar N. ; Fensterseifer, Isabel C. M. ; Faria-Junior, Celio ; Dias, Simoni C. ; Basak, Amit ; Hazra, Tapas K. ; Franco, Octávio L. (2015) Controlling resistant bacteria with a novel class of β-lactamase inhibitor peptides: from rational design to in vivo analyses Scientific Reports, 4 (1). ISSN 2045-2322

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Official URL: http://doi.org/10.1038/Srep06015

Related URL: http://dx.doi.org/10.1038/Srep06015

Abstract

Peptide rational design was used here to guide the creation of two novel short β-lactamase inhibitors, here named dBLIP-1 and -2, with length of five amino acid residues. Molecular modeling associated with peptide synthesis improved bactericidal efficacy in addition to amoxicillin, ampicillin and cefotaxime. Docked structures were consistent with calorimetric analyses against bacterial β-lactamases. These two compounds were further tested in mice. Whereas commercial antibiotics alone failed to cure mice infected with Staphylococcus aureus and Escherichia coli expressing β-lactamases, infection was cleared when treated with antibiotics in combination with dBLIPs, clearly suggesting that peptides were able to neutralize bacterial resistance. Moreover, immunological assays were also performed showing that dBLIPs were unable to modify mammalian immune response in both models, reducing the risks of collateral effects. In summary, the unusual peptides here described provide leads to overcome β-lactamase-based resistance, a remarkable clinical challenge.

Item Type:Article
Source:Copyright of this article belongs to Nature Publishing Group.
ID Code:129991
Deposited On:02 Dec 2022 06:03
Last Modified:05 Dec 2022 05:37

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