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AuthorKirchdoerfer, Robert N.
AuthorCottrell, Christopher A.
AuthorWang, Nianshuang
AuthorPallesen, Jesper
AuthorYassine, Hadi M.
AuthorTurner, Hannah L.
AuthorCorbett, Kizzmekia S.
AuthorGraham, Barney S.
AuthorMcLellan, Jason S.
AuthorWard, Andrew B.
Available date2016-07-21T10:20:49Z
Publication Date2015-03-03
Publication NameNature
Identifierhttp://dx.doi.org/10.1038/nature17200
Citation(yassine, Hadi., Kirchdoerfer, Robert N., / Pre-fusion structure of a human coronavirus spike protein , Nature Publishing Group, 531, 7592, Nature, 2015.
ISSN0028-0836
URIhttp://hdl.handle.net/10576/4686
AbstractHKU1 is a human betacoronavirus that causes mild yet prevalent respiratory disease1, and is related to the zoonotic SARS2 and MERS3 betacoronaviruses, which have high fatality rates and pandemic potential. Cell tropism and host range is determined in part by the coronavirus spike (S) protein4, which binds cellular receptors and mediates membrane fusion. As the largest known class I fusion protein, its size and extensive glycosylation have hindered structural studies of the full ectodomain, thus preventing a molecular understanding of its function and limiting development of effective interventions. Here we present the 4.0 Å resolution structure of the trimeric HKU1 S protein determined using singleparticle cryo-electron microscopy. In the pre-fusion conformation, the receptor-binding subunits, S1, rest above the fusion-mediating subunits, S2, preventing their conformational rearrangement. Surprisingly, the S1 C-terminal domains are interdigitated and form extensive quaternary interactions that occlude surfaces known in other coronaviruses to bind protein receptors. These features, along with the location of the two protease sites known to be important for coronavirus entry, provide a structural basis to support a model of membrane fusion mediated by progressive S protein destabilization through receptor binding and proteolytic cleavage. These studies should also serve as a foundation for the structure-based design of betacoronavirus vaccine immunogens.
SponsorNIH
Languageen
PublisherNature Publishing Group
SubjectCoronavirus
spike protein
structure
TitlePre-fusion structure of a human coronavirus spike protein
TypeArticle
Pagination118-121
Issue Number7592
Volume Number531
ESSN1476-4687
dc.accessType Abstract Only


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