Tailored design of protein nanoparticle scaffolds for multivalent presentation of viral glycoprotein antigens

糖蛋白 病毒 抗原呈递 病毒学 免疫系统 抗原 病毒蛋白 血凝素(流感) 表位 化学 细胞生物学 生物 生物化学 T细胞 免疫学
作者
George Ueda,Aleksandar Antanasijevic,Jorge A. Fallas,William Sheffler,Jeffrey Copps,Daniel Ellis,Geoffrey B. Hutchinson,Adam Moyer,Anila Yasmeen,Yaroslav Tsybovsky,Young‐Jun Park,Matthew J. Bick,Banumathi Sankaran,Rebecca A. Gillespie,Philip J. M. Brouwer,Peter H. Zwart,David Veesler,Masaru Kanekiyo,Barney S. Graham,Rogier W. Sanders,John P. Moore,Per Johan Klasse,Andrew B. Ward,Neil P. King,David Baker
出处
期刊:eLife [eLife Sciences Publications Ltd]
卷期号:9 被引量:144
标识
DOI:10.7554/elife.57659
摘要

Multivalent presentation of viral glycoproteins can substantially increase the elicitation of antigen-specific antibodies. To enable a new generation of anti-viral vaccines, we designed self-assembling protein nanoparticles with geometries tailored to present the ectodomains of influenza, HIV, and RSV viral glycoprotein trimers. We first de novo designed trimers tailored for antigen fusion, featuring N-terminal helices positioned to match the C termini of the viral glycoproteins. Trimers that experimentally adopted their designed configurations were incorporated as components of tetrahedral, octahedral, and icosahedral nanoparticles, which were characterized by cryo-electron microscopy and assessed for their ability to present viral glycoproteins. Electron microscopy and antibody binding experiments demonstrated that the designed nanoparticles presented antigenically intact prefusion HIV-1 Env, influenza hemagglutinin, and RSV F trimers in the predicted geometries. This work demonstrates that antigen-displaying protein nanoparticles can be designed from scratch, and provides a systematic way to investigate the influence of antigen presentation geometry on the immune response to vaccination.
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