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Virtual Screening Uncovers DspS Activators That Disperse Pseudomonas aeruginosa Biofilms
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    Virtual Screening Uncovers DspS Activators That Disperse Pseudomonas aeruginosa Biofilms
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    • Christabel Ming Ming Koh
      Christabel Ming Ming Koh
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
    • Siaw San Hwang
      Siaw San Hwang
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
    • Bee Theng Lau
      Bee Theng Lau
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
    • Enzo A. Palombo
      Enzo A. Palombo
      Department of Chemistry and Biotechnology, Swinburne University of Technology, Hawthorn, Victoria 3122, Australia
    • Irine Runnie Henry Ginjom
      Irine Runnie Henry Ginjom
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
    • Christopher Heng Xuan Ha
      Christopher Heng Xuan Ha
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
    • Taufiq Rahman
      Taufiq Rahman
      Department of Pharmacology, University of Cambridge, Tennis Court Road, Cambridge CB2 1PD, United Kingdom
    • Xavier Chee Wezen*
      Xavier Chee Wezen
      Faculty of Engineering, Computing, and Science, Swinburne University of Technology Sarawak, Kuching, Sarawak 93350, Malaysia
      Department of Biochemistry, Yong Loo Lin School of Medicine, National University of Singapore, Singapore 117596, Singapore
      *E-mail: [email protected]
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    ACS Infectious Diseases

    Cite this: ACS Infect. Dis. 2025, 11, 2, 413–429
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    https://doi.org/10.1021/acsinfecdis.4c00549
    Published October 18, 2024
    Copyright © 2024 American Chemical Society

    Abstract

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    Pseudomonas aeruginosa is the predominant bacterium found in many chronic biofilm infections. Over the past few decades, biofilm-related infections have posed a significant challenge to medical practice due to the increasing emergence of multidrug resistance. Cis-2-decenoic acid (CDA), a small molecule found in P. aeruginosa, has been shown to disperse biofilms formed by various bacteria and to work in synergy with common antibiotics. Despite that, the binding mechanism between CDA and the predicted cyclases/histidine kinases associated sensory extracellular (CHASE) domain of sensor protein DspS remains unknown in the absence of a crystallized protein structure. Moreover, the therapeutic potential of CDA is limited by its susceptibility to oxidative degradation and isomerization. In this work, we propose a structural model for the DspS CHASE domain. The resulting model displays an overall topology reminiscent of the sensor protein PcrK in Xanthomonas campestris. Through molecular dynamics simulations, a stable potential binding site for CDA was further identified. Virtual screening against the predicted site of DspS CHASE using our developed pipeline discovered two promising compounds, compounds 2 and 9, capable of dislodging 7-day P. aeruginosa biofilms at 50 μM without affecting bacterial growth. These compounds also enhanced the effects of ciprofloxacin against P. aeruginosa, reduced the survival of dispersed cells, and increased the expression of matrix-degrading enzyme genes pelA, pslG, and eddA. This study provides insights into CDA recognition by DspS and represents the first large-scale effort to uncover first-in-class DspS activators. At the same time, this work also underscores the effectiveness of a computational-aided drug discovery process in finding new activators, even without a known protein structure.

    Copyright © 2024 American Chemical Society

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    Supporting Information

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    The Supporting Information is available free of charge at https://pubs.acs.org/doi/10.1021/acsinfecdis.4c00549.

    • (a) Transmembrane helix position predictions; (b) Ramachandran plot for DspS CHASE structure; (c) CHASE domain alignments; (d) control docking results; (e) data for CDA and the top 10 compounds, including chemical and physicochemical properties, protein RMSD, ligand RMSD, MM/GBSA, final poses, and molecular interactions; (f) experimental data on PAO1 growth, biofilms, ciprofloxacin, and combination compounds on PAO1; (g) agarose gel electrophoresis results; and (h) purity data courtesy of the vendor Enamine Ltd. (PDF)

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    This article is cited by 1 publications.

    1. G. K. Wijesinghe, A. H. Nobbs, H. M. H. N. Bandara. The diffusible signaling factor family in microbial signaling: a current perspective. Critical Reviews in Microbiology 2025, 591 , 1-16. https://doi.org/10.1080/1040841X.2025.2457670

    ACS Infectious Diseases

    Cite this: ACS Infect. Dis. 2025, 11, 2, 413–429
    Click to copy citationCitation copied!
    https://doi.org/10.1021/acsinfecdis.4c00549
    Published October 18, 2024
    Copyright © 2024 American Chemical Society

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