Finding a peptide drug against MRSA

While L13 and L15 are unable to prevent S. aureus from growing, treating animals with the peptides in an infection model significantly reduced the pathogenicity of S. aureus.

In this respect, L15 and L13 cannot be considered antibiotics in the true sense of the word but anti-virulence compounds.

Interestingly, the genes for the biosynthesis of the Lpl proteins are present in all S. aureus strains investigated so far. The genes are clustered in a pathogenicity island which appears to be unique in S. aureus and some other pathogenic staphylococcal species. Therefore, the effects of L13 and L15 are limited to these species.

Epidemic and globally spreading S. aureus strains have a particularly high number of lpl orthologous genes. It is tempting to speculate that this gene cluster contributes to the rapid spreading of MRSA and MDRSA. Therefore, the two novel peptide drugs L13 and L15 could be employed to not only decrease S. aureus pathogenicity but also limit the spread of the epidemic strains.

Read the article “From a Hsp90 – binding protein to a peptide drug” by Ammanath et al. (2022).

(Source: FEMS Microbiology Blog) 

Friedrich Götz holds a Senior-professorship at the University Tübingen, Interfaculty Institute of Microbiology and Infection Medicine (IMIT) and is a member of the Cluster of Excellence 2124 ‘Controlling Microbes to Fight Infections’ (CMFI). His research interest includes the physiology of staphylococci and their interactions with humans.

Aparna Viswanathan Ammanath did her master’s studies at the Amrita Centre for Nanosciences and Molecular Medicine, Amrita University, Kerala, India. She is finishing her PhD in Microbial Genetics at the University Tübingen. Aparna studies mechanisms of new antimicrobial agents and works on new concepts for the development of targeted anti-infectives.