Abstract
AbstractVaricella-zoster virus (VZV) is a neurotropic alphaherpesvirus that causes
chickenpox and shingles. ORF7 is an important virulence determinant of VZV in both
human skin and nerve tissues, however, its specific function and involved molecular
mechanism in VZV pathogenesis remain largely elusive. Previous yeast two-hybrid
studies on intraviral protein-protein interaction network in herpesviruses have
revealed that VZV ORF7 may interact with ORF53, which is a virtually unstudied but
essential viral protein. The aim of this study is to identify and characterize VZV
ORF53, and to investigate its relationship with ORF7. For this purpose, we prepared
monoclonal antibodies against ORF53 and, for the first time, characterized it as a
~40 kDa viral protein predominantly localizing to the trans-Golgi network of the
infected host cell. Next, we further confirmed the interaction between ORF7 and
ORF53 by co-immunoprecipitation and co-localization studies in both
plasmid-transfected and VZV-infected cells. Moreover, interestingly, we found that
ORF53 lost its trans-Golgi network localization and became dispersed in the
cytoplasm of host cells infected with an ORF7-deleted recombinant VZV, and thus ORF7
seems to play a role in normal subcellular localization of ORF53. Collectively,
these results suggested that ORF7 and ORF53 may function as a complex during
infection, which may be implicated in VZV pathogenesis.
Subject
Virology,Molecular Medicine,Immunology
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