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Elucidation of unusual biosynthesis and DnaN-targeting mode of action of potent anti-tuberculosis antibiotics Mycoplanecins

Author

Listed:
  • Chengzhang Fu

    (Saarland University
    Helmholtz Center for Infection Research)

  • Yunkun Liu

    (Saarland University)

  • Christine Walt

    (Saarland University
    German Centre for Infection Research (DZIF))

  • Sari Rasheed

    (Saarland University
    German Centre for Infection Research (DZIF))

  • Chantal D. Bader

    (Saarland University
    German Centre for Infection Research (DZIF))

  • Peer Lukat

    (Helmholtz Centre for Infection Research)

  • Markus Neuber

    (Saarland University
    German Centre for Infection Research (DZIF))

  • F. P. Jake Haeckl

    (Saarland University
    German Centre for Infection Research (DZIF))

  • Wulf Blankenfeldt

    (Helmholtz Centre for Infection Research)

  • Olga V. Kalinina

    (Saarland University
    Helmholtz Institute for Pharmaceutical Research Saarland (HIPS), Helmholtz Centre for Infection Research (HZI), and Center for Bioinformatics, Saarland Informatics Campus)

  • Rolf Müller

    (Saarland University
    Helmholtz Center for Infection Research
    German Centre for Infection Research (DZIF))

Abstract

DNA polymerase III sliding clamp (DnaN) was recently validated as a new anti-tuberculosis target employing griselimycins. Three (2 S,4 R)−4-methylproline moieties of methylgriselimycin play significant roles in target binding and metabolic stability. Here, we identify the mycoplanecin biosynthetic gene cluster by genome mining using bait genes from the 4-methylproline pathway. We isolate and structurally elucidate four mycoplanecins comprising scarce homo-amino acids and 4-alkylprolines. Evaluating mycoplanecin E against Mycobacterium tuberculosis surprisingly reveals an excitingly low minimum inhibition concentration at 83 ng/mL, thus outcompeting griselimycin by approximately 24-fold. We show that mycoplanecins bind DnaN with nanomolar affinity and provide a co-crystal structure of mycoplanecin A-bound DnaN. Additionally, we reconstitute the biosyntheses of the unusual l-homoleucine, l-homonorleucine, and (2 S,4 R)−4-ethylproline building blocks by characterizing in vitro the full set of eight enzymes involved. The biosynthetic study, bioactivity evaluation, and drug target validation of mycoplanecins pave the way for their further development to tackle multidrug-resistant mycobacterial infections.

Suggested Citation

  • Chengzhang Fu & Yunkun Liu & Christine Walt & Sari Rasheed & Chantal D. Bader & Peer Lukat & Markus Neuber & F. P. Jake Haeckl & Wulf Blankenfeldt & Olga V. Kalinina & Rolf Müller, 2024. "Elucidation of unusual biosynthesis and DnaN-targeting mode of action of potent anti-tuberculosis antibiotics Mycoplanecins," Nature Communications, Nature, vol. 15(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-44953-5
    DOI: 10.1038/s41467-024-44953-5
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    References listed on IDEAS

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    1. Shota Atsumi & Taizo Hanai & James C. Liao, 2008. "Non-fermentative pathways for synthesis of branched-chain higher alcohols as biofuels," Nature, Nature, vol. 451(7174), pages 86-89, January.
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