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Bicyclic azetidines target acute and chronic stages of Toxoplasma gondii by inhibiting parasite phenylalanyl t-RNA synthetase

Author

Listed:
  • Joshua B. Radke

    (Washington University Sch. Med.)

  • Bruno Melillo

    (The Scripps Research Institute
    Broad Institute)

  • Payal Mittal

    (International Centre for Genetic Engineering and Biotechnology
    National Institute of Malaria Research)

  • Manmohan Sharma

    (International Centre for Genetic Engineering and Biotechnology)

  • Amit Sharma

    (International Centre for Genetic Engineering and Biotechnology
    National Institute of Malaria Research)

  • Yong Fu

    (Washington University Sch. Med.)

  • Taher Uddin

    (Washington University Sch. Med.)

  • Arthur Gonse

    (Broad Institute)

  • Eamon Comer

    (Broad Institute)

  • Stuart L. Schreiber

    (Broad Institute
    Harvard University)

  • Anil K. Gupta

    (The Scripps Research Institute
    Calibr at Scripps Research)

  • Arnab K. Chatterjee

    (The Scripps Research Institute
    Calibr at Scripps Research)

  • L. David Sibley

    (Washington University Sch. Med.)

Abstract

Toxoplasma gondii commonly infects humans and while most infections are controlled by the immune response, currently approved drugs are not capable of clearing chronic infection in humans. Hence, approximately one third of the world’s human population is at risk of reactivation, potentially leading to severe sequelae. To identify new candidates for treating chronic infection, we investigated a series of compounds derived from diversity-oriented synthesis. Bicyclic azetidines are potent low nanomolar inhibitors of phenylalanine tRNA synthetase (PheRS) in T. gondii, with excellent selectivity. Biochemical and genetic studies validate PheRS as the primary target of bicyclic azetidines in T. gondii, providing a structural basis for rational design of improved analogs. Favorable pharmacokinetic properties of a lead compound provide excellent protection from acute infection and partial protection from chronic infection in an immunocompromised mouse model of toxoplasmosis. Collectively, PheRS inhibitors of the bicyclic azetidine series offer promise for treatment of chronic toxoplasmosis.

Suggested Citation

  • Joshua B. Radke & Bruno Melillo & Payal Mittal & Manmohan Sharma & Amit Sharma & Yong Fu & Taher Uddin & Arthur Gonse & Eamon Comer & Stuart L. Schreiber & Anil K. Gupta & Arnab K. Chatterjee & L. Dav, 2022. "Bicyclic azetidines target acute and chronic stages of Toxoplasma gondii by inhibiting parasite phenylalanyl t-RNA synthetase," Nature Communications, Nature, vol. 13(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:13:y:2022:i:1:d:10.1038_s41467-022-28108-y
    DOI: 10.1038/s41467-022-28108-y
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