2012
DOI: 10.1128/jvi.06975-11
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Structural Basis of Rotavirus Strain Preference toward N -Acetyl- or N -Glycolylneuraminic Acid-Containing Receptors

Abstract: bThe rotavirus spike protein domain VP8* is essential for recognition of cell surface carbohydrate receptors, notably those incorporating N-acylneuraminic acids (members of the sialic acid family). N-Acetylneuraminic acids occur naturally in both animals and humans, whereas N-glycolylneuraminic acids are acquired only through dietary uptake in normal human tissues. The preference of animal rotaviruses for these natural N-acylneuraminic acids has not been comprehensively established, and detailed structural inf… Show more

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Cited by 40 publications
(62 citation statements)
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“…The VP8* domain of the RV outer capsid spike protein VP4 mediates this process (44), but the identity of VP8* receptors is quite controversial. It was believed that VP8* recognized either terminal sialic acid or internal sialic acid, mainly based on crystallographic and NMR studies (45)(46)(47)(48). However, recently a human strain (HAL1166) with a P [14] VP8* was found to bind to A-type histo-blood group antigen (49), a neonatal strain with a P [11] VP8* bound to type 2 precursor glycans (50), and several other P types recognized secretorrelated antigens Lewis b and H type 1 (51).…”
mentioning
confidence: 99%
“…The VP8* domain of the RV outer capsid spike protein VP4 mediates this process (44), but the identity of VP8* receptors is quite controversial. It was believed that VP8* recognized either terminal sialic acid or internal sialic acid, mainly based on crystallographic and NMR studies (45)(46)(47)(48). However, recently a human strain (HAL1166) with a P [14] VP8* was found to bind to A-type histo-blood group antigen (49), a neonatal strain with a P [11] VP8* bound to type 2 precursor glycans (50), and several other P types recognized secretorrelated antigens Lewis b and H type 1 (51).…”
mentioning
confidence: 99%
“…In all three cases, two hydrogen bonds are formed between protein residues and the extra hydroxyl group in Neu5Gc. Mutation of any of these residues results in a significant loss of activity of CRW-8 VP8 or SubB (35,39). In contrast to HPyV9, the binding site for Neu5Gc is more surface exposed in CRW-8 VP8 and STEC SubB, with one side of the ring facing the protein and the other side facing the solvent.…”
Section: Discussionmentioning
confidence: 99%
“…Similar to HPyV9 VP1, CRW-8 VP8 can bind both Neu5Ac and Neu5Gc, but it prefers the latter compound, which shows a higher binding affinity and results in increased cellular infectivity (39). Likewise, SubB can also bind Neu5Ac and Neu5Gc in glycan microarrays, but structural studies were successful only for the Neu5Gc complex, again indicating a preference for Neu5Gc binding (35).…”
Section: Discussionmentioning
confidence: 99%
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