๐ Coronavirus receptor switch explained from the stereochemistry of protein-carbohydrate interactions and a single mutation
Hemagglutinin-esterases (HEs) are bimodular envelope proteins of orthomyxoviruses, toroviruses, and coronaviruses with a carbohydrate-binding "lectin" domain appended to a receptordestroying sialate-O-acetylesterase ("esterase"). In concert, these domains facilitate dynamic virion attachment to cell-surface sialoglycans. Most HEs (type I) target 9-O-acetylated sialic acids (9-O-Ac-Sias), but one group of coronaviruses switched to using 4-O-Ac-Sias instead (type II). This specificity shift required quasisynchronous adaptations in the Sia-binding sites of both lectin and esterase domains. Previously, a partially disordered crystal structure of a type II HE revealed how the shift in lectin ligand specificity was achieved. How the switch in esterase substrate specificity was realized remained unresolved, however. Here, we present a complete structure of a type II HE with a receptor analog in the catalytic site and identify the mutations underlying the 9-O- to 4-O-Ac-Sia substrate switch. We show that (i) common principles pertaining to the stereochemistry of proteincarbohydrate interactions were at the core of the transition in lectin ligand and esterase substrate specificity; (ii) in consequence, the switch in O-Ac-Sia specificity could be readily accomplished via convergent intramolecular coevolution with only modest architectural changes in lectin and esterase domains; and (iii) a single, inconspicuous Ala-to-Ser substitution in the catalytic site was key to the emergence of the type II HEs. Our findings provide fundamental insights into how proteins "see" sugars and how this affects protein and virus evolution.
author
๐ค Bakkers, Mark J.G.
๐ค Zeng, Qinghong
๐ค Feitsma, Louris J.
๐ค Hulswit, Ruben J.G.
๐ค Li, Zeshi
๐ค Westerbeke, Aniek
๐ค Van Kuppeveld, Frank J.M.
๐ค Boons, Geert Jan
๐ค Langereis, Martijn A.
๐ค Huizinga, Eric G.
๐ค De Groot, Raoul J.
year
โฐ 2016
issn
๐ 10916490 00278424
volume
113
number
22
page
E3111-E3119
citedbycount
15
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