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Synthetic O-acetylated sialosides facilitate functional receptor identification for human respiratory viruses.

Nature chemistry (2021-03-24)
Zeshi Li, Yifei Lang, Lin Liu, Mehman I Bunyatov, Angelic Isaza Sarmiento, Raoul J de Groot, Geert-Jan Boons
RESUMEN

The transmission of viruses from animal reservoirs to humans poses major threats to public health. Preparedness for future zoonotic outbreaks requires a fundamental understanding of how viruses of animal origin have adapted to binding to a cell surface component and/or receptor of the new host. Here we report on the specificities of human and animal viruses that engage with O-acetylated sialic acid, which include betacoronaviruses, toroviruses and influenza C and D viruses. Key to these studies was the development of a chemoenzymatic methodology that can provide almost any sialate-acetylation pattern. A collection of O-acetylated sialoglycans was printed as a microarray for the determination of receptor specificity. These studies showed host-specific patterns of receptor recognition and revealed that three distinct human respiratory viruses uniquely bind 9-O-acetylated α2,8-linked disialoside. Immunofluorescence and cell entry studies support that such a glycotope as part of a ganglioside is a functional receptor for human coronaviruses.

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Anti-Mouse IgG (H+L), Biotin antibody produced in goat, ~2 mg/mL, affinity isolated antibody