Binding to sialic acids is not an essential step for the entry of animal rotaviruses to epithelial cells in culture.

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J Virol. 1993 September; 67(9): 5253-5259

Binding to sialic acids is not an essential step for the entry of animal rotaviruses to epithelial cells in culture.

E Méndez, C F Arias and S López

Departamento de Biología Molecular, Universidad Nacional Autónoma de México, Cuernavaca, Morelos.

ABSTRACT

The infection of target cells by animal rotaviruses requiresthe presence of sialic acids on the cell surface. Treatmentof the cells with neuraminidases or incubation of the viruseswith some sialoglycoproteins, such as glycophorin A, greatlyreduces virus binding, with the consequent reduction of viralinfectivity. In this work, we report the isolation of animalrotavirus variants whose infectivity is no longer dependenton the presence of sialic acids on the cell surface. In addition,although these variants bind to glycophorin A as efficientlyas the wild-type virus, this interaction no longer inhibit viralinfectivity. These observations indicate that the initial interactionof the mutants with the cell occurs at a site different fromthe sialic acid-binding site located on VP8, the smaller trypsincleavage product of VP4. Reassortant analysis showed that themutant phenotype segregates with the VP4 gene. Neutralizingmonoclonal antibodies directed to VP4 and VP7 were tested fortheir ability to neutralize the variants. Antibodies to VP7and VP5, the larger trypsin cleavage product of VP4, neutralizedthe mutants as efficiently as the wild-type virus. In contrast,although antibodies to VP8 were able to bind to the mutants,they showed little or no neutralizing activity. The implicationsof these findings in rotavirus attachment to and penetrationof epithelial cells in culture are discussed.

J Virol. 1993 September; 67(9): 5253-5259

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