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Secondary Metabolites Governing Microbiome Interaction of Staphylococcal Pathogens and Commensals

Journal

MICROBIAL PHYSIOLOGY
Volume 31, Issue 3, Pages 198-216

Publisher

KARGER
DOI: 10.1159/000517082

Keywords

Staphylococcus; Microbiome active compounds; Bacteriocins; Quorum sensing; Metallophores

Funding

  1. Deutsche Forschungsgemeinschaft (DFG, German Research Foundation) under Germany's Excellence Strategy [EXC 2124 - 390838134, GRK1708, TRR261, TRR156]
  2. German Center of Infection Research (DZIF)
  3. European Innovative Medicines Initiative IMI (COMBACTE)

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Various Staphylococcus species use secondary metabolites, such as bacteriocins and signaling molecules, to compete with other microorganisms in skin and upper airways. Understanding how these metabolites shape the fitness of Staphylococcus species in complex microbial and host defense contexts is a challenging field of future research. Harnessing these secondary metabolites could help exclude pathogenic species like Staphylococcus aureus from nasal microbiomes and aid in the development of anti-infective interventions.
Various Staphylococcus species colonize skin and upper airways of warm-blooded animals. They compete successfully with many other microorganisms under the hostile and nutrient-poor conditions of these habitats using mechanisms that we are only beginning to appreciate. Small-molecule mediators, whose biosynthesis requires complex enzymatic cascades, so-called secondary metabolites, have emerged as crucial components of staphylococcal microbiome interactions. Such mediators belong to a large variety of compound classes and several of them have attractive properties for future drug development. They include, for instance, bacteriocins such as lanthipeptides, thiopeptides, and fibupeptides that inhibit bacterial competitor species; signaling molecules such as thiolactone peptides that induce or inhibit sensory cascades in other bacteria; or metallophores such as staphyloferrins and staphylopine that scavenge scant transition metal ions. For some secondary metabolites such as the aureusimines, the exact function remains to be elucidated. How secondary metabolites shape the fitness of Staphylococcus species in the complex context of other microbial and host defense factors remains a challenging field of future research. A detailed understanding will help to harness staphylococcal secondary metabolites for excluding the pathogenic species Staphylococcus aureus from the nasal microbiomes of at-risk patients, and it will be instrumental for the development of advanced anti-infective interventions.

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