4.7 Article

Comparison of Proteomic Responses as Global Approach to Antibiotic Mechanism of Action Elucidation

Journal

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY
Volume 65, Issue 1, Pages -

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/AAC.01373-20

Keywords

antibiotic; chemical biology; mechanism of action; physiology; proteomics

Funding

  1. German Research Foundation [BA 4193/6-1]
  2. German Federal State of North Rhine-Westphalia
  3. National Institutes of Health [R01GM121650, NIAID/R01AI08093]
  4. NRW grant Translation of Innovative Antibiotics
  5. European Union
  6. European Regional Development Fund, Investing in Your Future (Innovative Antibiotics from the NRW)
  7. Research Infrastructure Center for System-Based Antibiotic Research [CESAR]
  8. SPIRIT Slovenija [P-MR-09/104]
  9. Ministry of Higher Education, Science, and Technology (Slovenian Research Agency, ARRS) [J4-8226, P4-0116]

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This study introduces a proteomic approach for rapid classification of new antibiotics, aiming to accelerate antibiotic research. Comparison of proteomic responses allows quick identification of antibiotics with dual mechanisms, and helps generate hypotheses on mechanisms of action. Proteomic profiling also reveals the impact of antibiotics on bacterial physiology.
New antibiotics are urgently needed to address the mounting resistance challenge. In early drug discovery, one of the bottlenecks is the elucidation of targets and mechanisms. To accelerate antibiotic research, we provide a proteomic approach for the rapid classification of compounds into those with precedented and unprecedented modes of action. We established a proteomic response library of Bacillus subtilis covering 91 antibiotics and comparator compounds, and a mathematical approach was developed to aid data analysis. Comparison of proteomic responses (CoPR) allows the rapid identification of antibiotics with dual mechanisms of action as shown for atypical tetracyclines. It also aids in generating hypotheses on mechanisms of action as presented for salvarsan (arsphenamine) and the antirheumatic agent auranofin, which is under consideration for repurposing. Proteomic profiling also provides insights into the impact of antibiotics on bacterial physiology through analysis of marker proteins indicative of the impairment of cellular processes and structures. As demonstrated for trans-translation, a promising target not yet exploited clinically, proteomic profiling supports chemical biology approaches to investigating bacterial physiology.

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