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Bacterial Toxin "Walks" Along MRSA and Kills It

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Published: November 4, 2019
 
| Original story from the University of Sheffield
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Scientists from the University of Sheffield have discovered how a potent bacterial toxin is able to target and kill MRSA, paving the way for potential new treatments for superbugs.

New research, led by Dr Stéphane Mesnage from the University of Sheffield, has explained how lysostaphin specifically recognizes MRSA cell walls and quickly causes the breakdown of this pathogen. The lysostaphin is able to increase the number of its molecules bound to the surface of the MRSA cell and this allows the enzyme to "walk" along the cell walls and cause rapid breakdown.

Lysostaphin is an enzyme that has been shown to eradicate Staphylococcal infections, such as MRSA, alone or in combination with antibiotics. Although it was discovered over 50 years ago, not much has been known about how it kills these infections.

The scientists hope to use their findings to develop new treatments for MRSA and other antibiotic-resistant superbugs that target the infection in a similar way.

MRSA is a bacterial superbug that is resistant to several antibiotics and frequently spreads in hospitals where people are more susceptible to infection.

Mesnage, Senior Lecturer in Molecular Biology and Biotechnology, said: "Lysostaphin is arguably the most studied enzyme after lysozyme, so we are delighted that our research is able to explain the mechanism underpinning its potent antibacterial activity.

"Our study explains how this enzyme is able to target and digest the MRSA bacteria and why it is so potent. Hospital-acquired infections caused by bacteria resistant to last-resort antibiotics are on the rise, but our work could lead to the development of new treatments for these superbugs that use the same targeting mechanism."

Reference

Mesnage et al. (2019) Two-site recognition of Staphylococcus aureus peptidoglycan by lysostaphin SH3b. Nature Chemical Biology. DOI: 10.1038/s41589-019-0393-4

This article has been republished from the following materials. Note: material may have been edited for length and content. For further information, please contact the cited source.

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