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Infectious parvovirus B19 circulates in the blood coated with active host protease inhibitors

Author

Listed:
  • Hyunwook Lee

    (University of Minnesota)

  • Ruben Assaraf

    (University of Bern
    Graduate School for Cellular and Biomedical Sciences)

  • Suriyasri Subramanian

    (The Pennsylvania State College of Medicine)

  • Dan Goetschius

    (The Pennsylvania State College of Medicine)

  • Jan Bieri

    (University of Bern)

  • Nadia M. DiNunno

    (The Pennsylvania State College of Medicine)

  • Remo Leisi

    (University of Bern)

  • Carol M. Bator

    (University of Minnesota)

  • Susan L. Hafenstein

    (University of Minnesota
    University of Minnesota
    Mayo Clinic)

  • Carlos Ros

    (University of Bern)

Abstract

The lack of a permissive cell culture system has limited high-resolution structures of parvovirus B19 (B19V) to virus-like particles (VLPs). In this study, we present the atomic resolution structure (2.2 Å) of authentic B19V purified from a patient blood sample. There are significant differences compared to non-infectious VLPs. Most strikingly, two host protease inhibitors (PIs), inter-alpha-trypsin inhibitor heavy chain 4 (ITIH4) and serpinA3, were identified in complex with the capsids in all patient samples tested. The ITIH4 binds specifically to the icosahedral fivefold axis and serpinA3 occupies the twofold axis. The protein-coated virions remain infectious, and the capsid-associated PIs retain activity; however, upon virion interaction with target cells, the PIs dissociate from the capsid prior to viral entry. Our finding of an infectious virion shielded by bound host serum proteins suggests an evolutionarily favored phenomenon to evade immune surveillance and escape host protease activity.

Suggested Citation

  • Hyunwook Lee & Ruben Assaraf & Suriyasri Subramanian & Dan Goetschius & Jan Bieri & Nadia M. DiNunno & Remo Leisi & Carol M. Bator & Susan L. Hafenstein & Carlos Ros, 2024. "Infectious parvovirus B19 circulates in the blood coated with active host protease inhibitors," Nature Communications, Nature, vol. 15(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-53794-1
    DOI: 10.1038/s41467-024-53794-1
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