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Structure and dynamics of an α-fucosidase reveal a mechanism for highly efficient IgG transfucosylation

Author

Listed:
  • Erik H. Klontz

    (University of Maryland School of Medicine
    University of Maryland School of Medicine
    University of Maryland School of Medicine)

  • Chao Li

    (University of Maryland)

  • Kyle Kihn

    (University of Maryland School of Pharmacy)

  • James K. Fields

    (University of Maryland School of Medicine
    University of Maryland School of Medicine
    University of Maryland School of Medicine)

  • Dorothy Beckett

    (University of Maryland)

  • Greg A. Snyder

    (University of Maryland School of Medicine)

  • Patrick L. Wintrode

    (University of Maryland School of Pharmacy)

  • Daniel Deredge

    (University of Maryland School of Pharmacy)

  • Lai-Xi Wang

    (University of Maryland)

  • Eric J. Sundberg

    (University of Maryland School of Medicine
    University of Maryland School of Medicine
    University of Maryland School of Medicine
    Emory University School of Medicine)

Abstract

Fucosylation is important for the function of many proteins with biotechnical and medical applications. Alpha-fucosidases comprise a large enzyme family that recognizes fucosylated substrates with diverse α-linkages on these proteins. Lactobacillus casei produces an α-fucosidase, called AlfC, with specificity towards α(1,6)-fucose, the only linkage found in human N-glycan core fucosylation. AlfC and certain point mutants thereof have been used to add and remove fucose from monoclonal antibody N-glycans, with significant impacts on their effector functions. Despite the potential uses for AlfC, little is known about its mechanism. Here, we present crystal structures of AlfC, combined with mutational and kinetic analyses, hydrogen–deuterium exchange mass spectrometry, molecular dynamic simulations, and transfucosylation experiments to define the molecular mechanisms of the activities of AlfC and its transfucosidase mutants. Our results indicate that AlfC creates an aromatic subsite adjacent to the active site that specifically accommodates GlcNAc in α(1,6)-linkages, suggest that enzymatic activity is controlled by distinct open and closed conformations of an active-site loop, with certain mutations shifting the equilibrium towards open conformations to promote transfucosylation over hydrolysis, and provide a potentially generalizable framework for the rational creation of AlfC transfucosidase mutants.

Suggested Citation

  • Erik H. Klontz & Chao Li & Kyle Kihn & James K. Fields & Dorothy Beckett & Greg A. Snyder & Patrick L. Wintrode & Daniel Deredge & Lai-Xi Wang & Eric J. Sundberg, 2020. "Structure and dynamics of an α-fucosidase reveal a mechanism for highly efficient IgG transfucosylation," Nature Communications, Nature, vol. 11(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-20044-z
    DOI: 10.1038/s41467-020-20044-z
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    Cited by:

    1. Bashar Shuoker & Michael J. Pichler & Chunsheng Jin & Hiroka Sakanaka & Haiyang Wu & Ana Martínez Gascueña & Jining Liu & Tine Sofie Nielsen & Jan Holgersson & Eva Nordberg Karlsson & Nathalie Juge & , 2023. "Sialidases and fucosidases of Akkermansia muciniphila are crucial for growth on mucin and nutrient sharing with mucus-associated gut bacteria," Nature Communications, Nature, vol. 14(1), pages 1-16, December.

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