| Literature DB >> 10891404 |
A Gedvilaite1, C Frömmel, K Sasnauskas, B Micheel, M Ozel, O Behrsing, J Staniulis, B Jandrig, S Scherneck, R Ulrich.
Abstract
We generated highly immunogenic virus-like particles that are based on the capsid protein VP1 of the hamster polyomavirus (HaPV-VP1) and harbor inserted foreign epitopes. The HaPV-VP1 regions spanning amino acids 81-88 (position 1), 222/223 (2), 244-246 (3), and 289-294 (4) were predicted to be surface exposed. An epitope of the pre-S1 region of the hepatitis B virus (designated S1; amino acid sequence DPAFR) was introduced into the predicted positions of VP1. All VP1/S1 fusion proteins were expressed in yeast and generated virus-like particles. Immunoassays using the S1-specific monoclonal antibody MA18/7 and immunization of C57Bl6 mice with different VP1/S1 constructs showed a pronounced reactivity and a strong S1-specific antibody response for particles carrying the insert in position 1, 2, 1+2, and 1+3. Our results suggest that HaPV-VP1 represents a highly flexible carrier moiety for the insertion of foreign sequences offering a broad range of potential uses, especially in vaccine development. Copyright 2000 Academic Press.Entities:
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Year: 2000 PMID: 10891404 DOI: 10.1006/viro.2000.0392
Source DB: PubMed Journal: Virology ISSN: 0042-6822 Impact factor: 3.616