Common Features of Enveloped Viruses and Implications for Immunogen Design for Next-Generation Vaccines

Publication date: 8 March 2018 Source:Cell, Volume 172, Issue 6 Author(s): Felix A. Rey, Shee-Mei Lok Enveloped viruses enter cells by inducing fusion of viral and cellular membranes, a process catalyzed by a specialized membrane-fusion protein expressed on their surface. This review focuses on recent structural studies of viral fusion proteins with an emphasis on their metastable prefusion form and on interactions with neutralizing antibodies. The fusion glycoproteins have been difficult to study because they are present in a labile, metastable form at the surface of infectious virions. Such metastability is a functional requirement, allowing these proteins to refold into a lower energy conformation while transferring the difference in energy to catalyze the membrane fusion reaction. Structural studies have shown that stable immunogens presenting the same antigenic sites as the labile wild-type proteins efficiently elicit potently neutralizing antibodies, providing a framework with which to engineer the antigens for stability, as well as identifying key vulnerability sites that can be used in next-generation subunit vaccine design. Teaser A greater understanding of how viruses fuse with host cells, driven by recent advances in viral structural biology, is leading the way for new immunogen design and vaccine development.
Source: Cell - Category: Cytology Source Type: research
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