Heterologous Sarbecovirus Receptor Binding Domains as Scaffolds for SARS-CoV-2 Receptor Binding Motif Presentation

被引:0
作者
Hauser, Blake M. [1 ]
Sangesland, Maya [1 ]
Lam, Evan C. [1 ]
St Denis, Kerri J. [1 ]
Sheehan, Maegan L. [1 ]
Vu, Mya L. [1 ]
Cheng, Agnes H. [1 ]
Sordilla, Sophia [1 ]
Lamson, Dana Thornlow [1 ,2 ]
Almawi, Ahmad W. [3 ]
Balazs, Alejandro B. [1 ]
Lingwood, Daniel [1 ]
Schmidt, Aaron G. [1 ,2 ]
机构
[1] MIT & Harvard, Ragon Inst Mass Gen, Cambridge, MA 02139 USA
[2] Harvard Med Sch, Dept Microbiol, Boston, MA 02115 USA
[3] Harvard Med Sch, Ctr Mol Interact, Dept Biol Chem & Mol Pharmacol, Boston, MA 02115 USA
关键词
SARS-CoV-2; coronavirus; immune imprinting; STRUCTURE-BASED DESIGN; NANOPARTICLE VACCINES; IMMUNE-RESPONSES; PROTEIN; ANTIBODIES; EPITOPE; SPIKE; RBD; ELICITATION; MERS;
D O I
10.1021/acsinfecdis.3c00483
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Structure-guided rational immunogen design can generate optimized immunogens that elicit a desired humoral response. Design strategies often center on targeting conserved sites on viral glycoproteins that will ultimately confer potent neutralization. For SARS-CoV-2 (SARS-2), the surface-exposed spike glycoprotein includes a broadly conserved portion, the receptor binding motif (RBM), that is required to engage the host cellular receptor, ACE2. Expanding humoral responses to this site may result in a more potent neutralizing antibody response against diverse sarbecoviruses. Here, we used a "resurfacing" approach and iterative design cycles to graft the SARS-2 RBM onto heterologous sarbecovirus scaffolds. The scaffolds were selected to vary the antigenic distance relative to SARS-2 to potentially focus responses to RBM. Multimerized versions of these immunogens elicited broad neutralization against sarbecoviruses in the context of preexisting SARS-2 immunity. These validated engineering approaches can help inform future immunogen design efforts for sarbecoviruses and are generally applicable to other viruses.
引用
收藏
页码:553 / 561
页数:9
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