Thermophilic Filamentous Fungus C1-Cell-Cloned SARS-CoV-2-Spike-RBD-Subunit-Vaccine Adjuvanted with Aldydrogel (R) 85 Protects K18-hACE2 Mice against Lethal Virus Challenge

Vaccines(2022)

Cited 4|Views16
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Abstract
SARS-CoV-2 is evolving with increased transmission, host range, pathogenicity, and virulence. The original and mutant viruses escape host innate (Interferon) immunity and adaptive (Antibody) immunity, emphasizing unmet needs for high-yield, commercial-scale manufacturing to produce inexpensive vaccines/boosters for global/equitable distribution. We developed DYAI-100A85, a SARS-CoV-2 spike receptor binding domain (RBD) subunit antigen vaccine expressed in genetically modified thermophilic filamentous fungus, Thermothelomyces heterothallica C1, and secreted at high levels into fermentation medium. The RBD-C-tag antigen strongly binds ACE2 receptors in vitro. Alhydrogel (R)'85'-adjuvanted RDB-C-tag-based vaccine candidate (DYAI-100A85) demonstrates strong immunogenicity, and antiviral efficacy, including in vivo protection against lethal intranasal SARS-CoV-2 (D614G) challenge in human ACE2-transgenic mice. No loss of body weight or adverse events occurred. DYAI-100A85 also demonstrates excellent safety profile in repeat-dose GLP toxicity study. In summary, subcutaneous prime/boost DYAI-100A85 inoculation induces high titers of RBD-specific neutralizing antibodies and protection of hACE2-transgenic mice against lethal challenge with SARS-CoV-2. Given its demonstrated safety, efficacy, and low production cost, vaccine candidate DYAI-100 received regulatory approval to initiate a Phase 1 clinical trial to demonstrate its safety and efficacy in humans.
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COVID-19,antigen,pandemic,SARS-CoV-2,receptor binding domain,RBD,vaccine,biomanufacturing,dyadic,zoonotic,variants of concern,Thermothelomyces heterothallica,Myceliophthora thermophila,CHO-cell,insect cells,baculovirus,neutralizing antibodies,recombinant protein subunit vaccine,toxicology,glycoprotein,glycosylation,glycans,efficacy,stability,adjuvant,alum,aluminum-based vaccine adjuvants,C-tag,BALB/c mice,K18-hACE-2 mice,intranasal challenge,virus,IgG,IgG1 and IgG2b
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