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Influence of glycosylation and oligomerization of vaccinia virus complement control protein on level and pattern of functional activity and immunogenicity

摘要Vaccinia virus complement control protein(VCP)is one of the proteins encoded by vaccinia virus to modulate the host inflammatory response.VCP modulates the inflammatory response and protects viral habitat by inhibiting the classical and the alternative pathways of complement activation.The extended structure of VCP,mobility between its sequential domains,charge distribution and type of residues at the binding regions are factors that have been identified to influence its ability to bind to complement proteins.We report that a Lister strain of vaccinia virus encodes a VCP homolog(Lis VCP)that is functional,glycosylated,has two amino acids less than the well-characterized VCP from vaccinia virus WR strain(WR VCP),and the human smallpox inhibitor of complement enzymes(SPICE)from variola virus.The glycosylated VCP of Lister is immunogenic in contrast to the weak immunogenicity of the nonglycosylated VCP.Lis VCP is the only orthopoxviral VCP homolog found to be glycosylated,and we speculate that glycosylation influences its pattern of complement inhibition.We also correlate dimerization of VCP observed only in mammalian and baculovirus expression systems to higher levels of activity than monomers,observed in the yeast expression system.

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作者单位 Department of Pharmaceutical Sciences,Sullivan University College of Pharmacy,Louisville,KY,USA [1]
DOI 10.1007/s13238-010-0139-2
发布时间 2011-04-07(万方平台首次上网日期,不代表论文的发表时间)
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蛋白质与细胞

蛋白质与细胞

2010年01卷12期

1084-1092页

SCIMEDLINEISTICCSCDCABP

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