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Heterologous vs. homologous vaccine regimens: Sulfated lactosyl archaeol (SLA) archaeosome-adjuvanted SARS-CoV-2 spike protein boost following an mRNA/LNP prime induces robust and balanced immune responses

Vaccine. 2026-02; 
Tyler M Renner, Gerard Agbayani, Hiva Azizi, Lise Deschatelets, Renu Dudani, Blair A Harrison, Usha D Hemraz, Roger Koukiekolo, Matthew Stuible, Yves Durocher, Michael J McCluskie, Bassel Akache
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Codon Optimization the SARS-CoV-2 reference strain spike ectodomain sequence (amino acids 1–1208 derived from Genbank accession number MN908947) was codon-optimized for Chinese Hamster Ovary (CHO) cells and synthesized by GenScript. The plasmid DNA templates used to generate the tested mRNAs were designed based on the publicly available Pfizer-BioNTech mRNA/LNP vaccine sequence [55] and synthesized by Genscript (Piscataway, NJ, USA) in a pUC57 backbone, as described previously. Get A Quote
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Abstract

To combat the spread of and disease caused by SARS-CoV-2, mRNA/LNP vaccines were introduced into the clinic in 2020 with tremendous uptake and success. Since then, there have been multiple other SARS-CoV-2 vaccines approved across different countries based on various types of platforms including viral vector, inactivated virus and adjuvanted protein subunit vaccines. This has led to a scenario where there is a high probability of heterologous vaccinations in certain populations, whereby booster doses will differ from the initial vaccine formulations they received. We have previously demonstrated the immunogenicity of sulfated lactosyl archaeol (SLA) archaeosome-adjuvanted protein subunit vaccines and mRNA/LNPs ... More

Keywords

Adjuvant; Archaeosome; Glycolipid; Heterologous; Homologous; SARS-CoV-2; Subunit vaccine; Sulfated lactosyl archaeol (SLA); mRNA vaccine.