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Exploiting the aggregation propensity of beta-lactamases to design inhibitors that induce enzyme misfolding

Medicine and Health

Exploiting the aggregation propensity of beta-lactamases to design inhibitors that induce enzyme misfolding

L. Khodaparast, L. Khodaparast, et al.

This groundbreaking research conducted by Ladan Khodaparast, Laleh Khodaparast, and their colleagues reveals a novel approach to combat antibiotic resistance via the aggregation of beta-lactamases. By utilizing synthetic peptides to induce enzyme misfolding, the study paves the way for restoring antibiotic sensitivity in resistant strains, addressing a pressing global health crisis.... show more
Abstract
There is an arms race between beta-lactam antibiotics development and co-evolving beta-lactamases, which provide resistance by breaking down beta-lactam rings. We have observed that certain beta-lactamases tend to aggregate, which persists throughout their evolution under the selective pressure of antibiotics on their active sites. Interestingly, we find that existing beta-lactamase active site inhibitors can act as molecular chaperones, promoting the proper folding of these resistance factors. Therefore, we have created Pept-Ins, synthetic peptides designed to exploit the structural weaknesses of beta-lactamases by causing them to misfold into intracellular inclusion bodies. This approach restores sensitivity to a wide range of beta-lactam antibiotics in resistant clinical isolates, including those with Extended Spectrum variants that pose significant challenges in medical practice. Our findings suggest that targeted aggregation of resistance factors could offer a strategy for identifying molecules that aid in addressing the global antibiotic resistance crisis.
Publisher
Nature Communications
Published On
Sep 09, 2023
Authors
Ladan Khodaparast, Laleh Khodaparast, Guiqin Wu, Emiel Michiels, Rodrigo Gallardo, Bert Houben, Teresa Garcia, Matthias De Vleeschouwer, Meine Ramakers, Hannah Wilkinson, Ramon Duran-Romaña, Johan Van Eldere, Frederic Rousseau, Joost Schymkowitz
Tags
antibiotic resistance
beta-lactamases
synthetic peptides
enzyme aggregation
antibiotic sensitivity
clinical isolates
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