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Structural and mechanistic basis for translation inhibition by macrolide and ketolide antibiotics

Author

Listed:
  • Bertrand Beckert

    (University of Hamburg)

  • Elodie C. Leroy

    (Institut Européen de Chimie et Biologie)

  • Shanmugapriya Sothiselvam

    (University of Illinois at Chicago)

  • Lars V. Bock

    (Max Planck Institute for Biophysical Chemistry)

  • Maxim S. Svetlov

    (University of Illinois at Chicago)

  • Michael Graf

    (University of Hamburg)

  • Stefan Arenz

    (University of Hamburg)

  • Maha Abdelshahid

    (University of Hamburg)

  • Britta Seip

    (Institut Européen de Chimie et Biologie)

  • Helmut Grubmüller

    (Max Planck Institute for Biophysical Chemistry)

  • Alexander S. Mankin

    (University of Illinois at Chicago)

  • C. Axel Innis

    (Institut Européen de Chimie et Biologie)

  • Nora Vázquez-Laslop

    (University of Illinois at Chicago)

  • Daniel N. Wilson

    (University of Hamburg)

Abstract

Macrolides and ketolides comprise a family of clinically important antibiotics that inhibit protein synthesis by binding within the exit tunnel of the bacterial ribosome. While these antibiotics are known to interrupt translation at specific sequence motifs, with ketolides predominantly stalling at Arg/Lys-X-Arg/Lys motifs and macrolides displaying a broader specificity, a structural basis for their context-specific action has been lacking. Here, we present structures of ribosomes arrested during the synthesis of an Arg-Leu-Arg sequence by the macrolide erythromycin (ERY) and the ketolide telithromycin (TEL). Together with deep mutagenesis and molecular dynamics simulations, the structures reveal how ERY and TEL interplay with the Arg-Leu-Arg motif to induce translational arrest and illuminate the basis for the less stringent sequence-specific action of ERY over TEL. Because programmed stalling at the Arg/Lys-X-Arg/Lys motifs is used to activate expression of antibiotic resistance genes, our study also provides important insights for future development of improved macrolide antibiotics.

Suggested Citation

  • Bertrand Beckert & Elodie C. Leroy & Shanmugapriya Sothiselvam & Lars V. Bock & Maxim S. Svetlov & Michael Graf & Stefan Arenz & Maha Abdelshahid & Britta Seip & Helmut Grubmüller & Alexander S. Manki, 2021. "Structural and mechanistic basis for translation inhibition by macrolide and ketolide antibiotics," Nature Communications, Nature, vol. 12(1), pages 1-15, December.
    • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-24674-9
    DOI: 10.1038/s41467-021-24674-9
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    Cited by:

    1. Corentin R. Fostier & Farès Ousalem & Elodie C. Leroy & Saravuth Ngo & Heddy Soufari & C. Axel Innis & Yaser Hashem & Grégory Boël, 2023. "Regulation of the macrolide resistance ABC-F translation factor MsrD," Nature Communications, Nature, vol. 14(1), pages 1-15, December.
    2. Chih-Wei Chen & Nadja Leimer & Egor A. Syroegin & Clémence Dunand & Zackery P. Bulman & Kim Lewis & Yury S. Polikanov & Maxim S. Svetlov, 2023. "Structural insights into the mechanism of overcoming Erm-mediated resistance by macrolides acting together with hygromycin-A," Nature Communications, Nature, vol. 14(1), pages 1-13, December.

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