Literature DB >> 35746695

New p35 (H3L) Epitope Involved in Vaccinia Virus Neutralization and Its Deimmunization.

Yana Khlusevich1, Andrey Matveev1, Lyudmila Emelyanova1, Elena Goncharova2, Natalia Golosova1, Ivan Pereverzev3, Nina Tikunova1.   

Abstract

Vaccinia virus (VACV) is a promising oncolytic agent because it exhibits many characteristic features of an oncolytic virus. However, its effectiveness is limited by the strong antiviral immune response induced by this virus. One possible approach to overcome this limitation is to develop deimmunized recombinant VACV. It is known that VACV p35 is a major protein for B- and T-cell immune response. Despite the relevance of p35, its epitope structure remains insufficiently studied. To determine neutralizing epitopes, a panel of recombinant p35 variants was designed, expressed, and used for mice immunization. Plaque-reduction neutralization tests demonstrated that VACV was only neutralized by sera from mice that were immunized with variants containing both N- and C- terminal regions of p35. This result was confirmed by the depletion of anti-p35 mice sera with recombinant p35 variants. At least nine amino acid residues affecting the immunogenic profile of p35 were identified. Substitutions of seven residues led to disruption of B-cell epitopes, whereas substitutions of two residues resulted in the recognition of the mutant p35 solely by non-neutralizing antibodies.

Entities:  

Keywords:  H3L; deimmunization; epitope; immunogenicity; neutralizing antibodies; oncolytic vaccinia virus; oncolytic virus; orthopoxvirus; p35; vaccinia virus

Mesh:

Substances:

Year:  2022        PMID: 35746695      PMCID: PMC9227246          DOI: 10.3390/v14061224

Source DB:  PubMed          Journal:  Viruses        ISSN: 1999-4915            Impact factor:   5.818


  58 in total

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