4.7 Article

Proteome of Staphylococcus aureus Biofilm Changes Significantly with Aging

Journal

Publisher

MDPI
DOI: 10.3390/ijms23126415

Keywords

Staphylococcus aureus; biofilms; proteome; TMT; mass spectrometry; aging; metabolic processes; biosynthetic processes; transport systems; stress responses

Funding

  1. Macquarie University [44705980]
  2. Australian Proteome Analysis Facility, Macquarie University, Australia

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Staphylococcus aureus, a pathogenic bacterium capable of forming biofilms, is frequently found in infections related to implanted medical devices. This study used high-throughput mass spectrometry to analyze changes in the proteome of S. aureus biofilms grown for different durations. The results revealed significant alterations in the protein profiles of 3-day and 12-day biofilms compared to planktonic growth at 24 hours. These findings shed light on the role of specific proteins in biofilm development, potentially leading to new therapeutic strategies for biofilm-related implant infections.
Staphylococcus aureus is a notorious biofilm-producing pathogen that is frequently isolated from implantable medical device infections. As biofilm ages, it becomes more tolerant to antimicrobial treatment leading to treatment failure and necessitating the costly removal of infected devices. In this study, we performed in-solution digestion followed by TMT-based high-throughput mass spectrometry and investigated what changes occur in the proteome of S. aureus biofilm grown for 3-days and 12-days in comparison with 24 h planktonic. It showed that proteins associated with biosynthetic processes, ABC transporter pathway, virulence proteins, and shikimate kinase pathway were significantly upregulated in a 3-day biofilm, while proteins associated with sugar transporter, degradation, and stress response were downregulated. Interestingly, in a 3-day biofilm, we observed numerous proteins involved in the central metabolism pathways which could lead to biofilm growth under diverse environments by providing an alternative metabolic route to utilize energy. In 12-day biofilms, proteins associated with peptidoglycan biosynthesis, sugar transporters, and stress responses were upregulated, whereas proteins associated with ABC transporters, DNA replication, and adhesion proteins were downregulated. Gene Ontology analysis revealed that more proteins are involved in metabolic processes in 3dwb compared with 12dwb. Furthermore, we observed significant variations in the formation of biofilms resulting from changes in the level of metabolic activity in the different growth modes of biofilms that could be a significant factor in S. aureus biofilm maturation and persistence. Collectively, potential marker proteins were identified and further characterized to understand their exact role in S. aureus biofilm development, which may shed light on possible new therapeutic regimes in the treatment of biofilm-related implant-associated infections.

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