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Fragment-based drug nanoaggregation reveals drivers of self-assembly

Author

Listed:
  • Chen Chen

    (Memorial Sloan Kettering Cancer Center
    Weill Cornell Medicine
    Memorial Sloan Kettering Cancer Center)

  • You Wu

    (Memorial Sloan Kettering Cancer Center
    Weill Cornell Medicine
    Memorial Sloan Kettering Cancer Center)

  • Shih-Ting Wang

    (Brookhaven National Laboratory)

  • Naxhije Berisha

    (Memorial Sloan Kettering Cancer Center
    The Graduate Center of the City University of New York
    City University of New York)

  • Mandana T. Manzari

    (Memorial Sloan Kettering Cancer Center
    Kaleidoscope Technologies, Inc.)

  • Kristen Vogt

    (Memorial Sloan Kettering Cancer Center
    Weill Cornell Medicine
    Memorial Sloan Kettering Cancer Center)

  • Oleg Gang

    (Brookhaven National Laboratory
    Columbia University
    Columbia University)

  • Daniel A. Heller

    (Memorial Sloan Kettering Cancer Center
    Weill Cornell Medicine
    Memorial Sloan Kettering Cancer Center)

Abstract

Drug nanoaggregates are particles that can deleteriously cause false positive results during drug screening efforts, but alternatively, they may be used to improve pharmacokinetics when developed for drug delivery purposes. The structural features of molecules that drive nanoaggregate formation remain elusive, however, and the prediction of intracellular aggregation and rational design of nanoaggregate-based carriers are still challenging. We investigate nanoaggregate self-assembly mechanisms using small molecule fragments to identify the critical molecular forces that contribute to self-assembly. We find that aromatic groups and hydrogen bond acceptors/donors are essential for nanoaggregate formation, suggesting that both π-π stacking and hydrogen bonding are drivers of nanoaggregation. We apply structure-assembly-relationship analysis to the drug sorafenib and discover that nanoaggregate formation can be predicted entirely using drug fragment substructures. We also find that drug nanoaggregates are stabilized in an amorphous core-shell structure. These findings demonstrate that rational design can address intracellular aggregation and pharmacologic/delivery challenges in conventional and fragment-based drug development processes.

Suggested Citation

  • Chen Chen & You Wu & Shih-Ting Wang & Naxhije Berisha & Mandana T. Manzari & Kristen Vogt & Oleg Gang & Daniel A. Heller, 2023. "Fragment-based drug nanoaggregation reveals drivers of self-assembly," Nature Communications, Nature, vol. 14(1), pages 1-12, December.
    • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-43560-0
    DOI: 10.1038/s41467-023-43560-0
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    References listed on IDEAS

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    1. Aviram Mizrachi & Yosi Shamay & Janki Shah & Samuel Brook & Joanne Soong & Vinagolu K. Rajasekhar & John L. Humm & John H. Healey & Simon N. Powell & José Baselga & Daniel A. Heller & Adriana Haimovit, 2017. "Tumour-specific PI3K inhibition via nanoparticle-targeted delivery in head and neck squamous cell carcinoma," Nature Communications, Nature, vol. 8(1), pages 1-10, April.
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