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J. Virol., 11 1997, 8213-8220, Vol 71, No. 11
M Ciarlet, Y Hoshino and F Liprandi
A panel of single and double neutralization-resistant escape mutants of
serotype G11 porcine rotavirus strains A253 and YM, selected with G11
monotype- and serotype-specific neutralizing monoclonal antibodies (MAbs)
to VP7, was tested in neutralization assays with hyperimmune sera raised
against rotavirus strains of different serotypes. Escape mutants with an
amino acid substitution in antigenic region A (amino acids [aa] 87 to 101)
resulting in a residue identical or chemically similar to those present at
the same positions in serotype G3 strains, at positions 87 for strain A253
and 96 for strain YM, were significantly more sensitive than the parental
strains to neutralization with sera against some serotype G3 strains. Also,
one YM antigenic variant (YM-5E6.1) acquired reactivity by enzyme-linked
immunosorbent assay with MAbs 159, 57/8, and YO-1E2, which react with G3
strains, but not with the serotype G11 parental strain YM. Cross-
adsorption studies suggested that the observed cross-neutralization by the
G3-specific sera was due to the sera containing antibodies reactive with
the parental strain plus antibodies reactive with the epitope(s) on the
antigenic variant that mimick the serotype G3 specific one(s). Moreover,
antibodies reactive with antigenic region F (aa 235 to 242) of VP7 might
also be involved since cross-reactivity to serotype G3 was decreased in
double mutants carrying an additional mutation, which creates a potential
glycosylation site at position 238. Thus, single point mutations can affect
the serotype reactivity of G11 porcine rotavirus strains with both
monoclonal and polyclonal antibodies and may explain the origin of
rotavirus strains with dual serotype specificity based on sequence
divergence of VP7.
Copyright © 1997, American Society for Microbiology
Single point mutations may affect the serotype reactivity of serotype G11 porcine rotavirus strains: a widening spectrum?
Laboratorio de Biologia de Virus, Centro de Microbiologia y Biologia Celular, Instituto Venezolano de Investigaciones Cientificas, Caracas, Venezuela. mciarlet@melnick.mvir.bcm.tmc.edu
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