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Induction of Broadly Cross-Reactive Antibody Responses to SARS-CoV-2 Variants by S1 Nanoparticle Vaccines

J Virol. 2022-07; 
Cong Sun , Run-Yu Yuan , Chu Xie , Jiu-Feng Sun , Xin-Yan Fang , Yi-Sha Hu , Xiao-Hui Yu, Zheng Liu , Mu-Sheng Zeng , Yin-Feng Kang
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Gene Synthesis The gene fragments encoding SARS-CoV-2 S1 (residues 16 to 685, GenBank no. MN908947) and human ACE2 (residues 19 to 615, GenBank no. NM_021804) were codon optimized for human cells and synthesized by GenScript, and then they were cloned into mammalian expression vector VRC8400 using a single restriction site (BamHI). Then, endotoxin was removed using ToxinEraser endotoxin removal kit (GenScript) according to the manufacturer’s protocol. Get A Quote
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摘要

Despite the rapid deployment of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) vaccines, the emergence of SARS-CoV-2 variants and reports of their immune evasion characteristics have led to an urgent need for novel vaccines that confer potent cross-protective immunity. In this study, we constructed three different SARS-CoV-2 spike S1-conjugated nanoparticle vaccine candidates that exhibited high structural homogeneity and stability. Notably, these vaccines elicited up to 50-times-higher neutralizing antibody titers than the S1 monomer in mice. Crucially, it was found that the S1-conjugated nanoparticle vaccine could elicit comparable levels of neutralizing antibodies against wild-type or emerging ... More

關鍵詞

Omicron; S1; SARS-CoV-2; nanoparticle vaccine; variants of concern.
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