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Structure of the human astrovirus capsid spike in complex with the neonatal Fc receptor

Nature Communications. 2025-11; 
Adam Lentz, Sarah Lanning, Khurshid R Iranpur, Lena Ricemeyer, Carlos F Arias, Rebecca M DuBois Department of Biomolecular Engineering, University of California Santa Cruz, Santa Cruz
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Mutagenesis Services HAstV1 Y475A and 3 A mutant spike plasmids were generated by GenScript. HAstV1 K467H spike mutant plasmid was cloned by GenScript into the pET52b + expression vector in-frame with a C-terminal Avitag for directed biotinylation for acidic pH binding studies. Get A Quote

摘要

Human astroviruses (HAstVs) are a leading cause of viral gastroenteritis in children worldwide. Recently the neonatal Fc receptor (FcRn) was identified as a receptor for HAstV, however the molecular basis for the FcRn-HAstV interaction remained unclear. Here, we report the crystal structure of FcRn bound to the HAstV capsid spike domain at 3.4 angstroms resolution. We show that all classical HAstV spikes bind to FcRn and we identify three conserved HAstV spike residues that mediate binding to FcRn. Using competition binding assays, we show that the HAstV spike competes with IgG for binding to FcRn. Additionally, we demonstrate that the FcRn inhibitor, nipocalimab, and anti-HAstV neutralizing monoclonal antibodi... More

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