CONICET | Buscador de Institutos y Recursos Humanos

Varicella-Zoster virus (VZV), a neurotropic alphaherpesvirus, causes chickenpox upon primaryinfection and shingles after reactivation from latency. VZV ORF25, the orthologue of UL33 in Herpes Simplex virus(HSV), is a 156 aminoacid (aa) protein with a C-terminal region that is highly conserved among all herpesviruses.Little is known about ORF25 functions, but recent work in HSV has suggested a role in DNA packaging.We haveperformed a PCR mutagenesis strategy to construct nine different aa-to-alanine substitution mutants within theconserved C-terminal region of ORF25. All nine aa substitution mutants, a wildtype revertant mutant, a revertantmutant containing a synthetic ORF25 gene variant, and a complete deletion mutant of ORF25 were analyzedfor their ability to reconstitute recombinant VZV by utilizing the cosmid system technology. So far, both wildtyperevertant mutants and three ORF25 aa substitution mutants, namely: PP 82/83 AA, VV 123/124 AA, and TRRR133-136 AAAA, were able to reconstitute infectious viruses. At least one ORF25 aa substitution mutant virus showsa phenotype of attenuated growth and smaller plaques. ORF25 seems to be essential for VZV replication, sinceno infectious virus could be reconstituted from the deletion mutant of ORF25.ORF25 comprises a cytoplasmiclocalization when expressed alone, but translocates to the nucleus in virally infected cells, as we could demonstrateby immunofluorescence microscopy with a polyclonal rabbit antiserum.To identify viral binding partners of ORF25,we have performed a comprehensive yeast-two-hybrid (Y2H) analysis of N- and C-terminal mutants of ORF25against a library of VZV proteins.These Y2H analyses indicate that ORF25 interacts with itself at its C-terminus andwith other viral (mainly tegument) proteins at its N-terminus. The strong interaction of ORF25 with the tegumentproteins: ORF63, ORF47, and ORF66 (HSV: ICP22, UL13, and US3) could be reproduced in a LUMIER-basedscreening system in 293 cells.

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