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Mechanistic insights into the structure-based design of a CspZ-targeting Lyme disease vaccine

Nature Communications. 2025-04; 
Kalvis Brangulis, Jill Malfetano, Ashley L. Marcinkiewicz, Alan Wang, Yi-Lin Chen, Jungsoon Lee, Zhuyun Liu, Xiuli Yang, Ulrich Strych, Dagnija Tupina, Inara Akopjana, Maria-Elena Bottazzi, Utpal Pal, Ching-Lin Hsieh, Wen-Hsiang Chen & Yi-Pin Lin NYSDOH, Tufts University, SUNY Albany
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Gene Synthesis The DNA encoding untagged CspZ and its derived mutant proteins were codon-optimized based on E. coli codon usage preference, synthesized, and subcloned into the pET41a using NdeI/XhoI sites by GenScript (Piscataway, NJ). These two mAbs were further humanized and chimerized using the service provided by GenScript Probio (Piscataway, NJ). Get A Quote

摘要

Borrelia burgdorferi (Bb) causes Lyme disease (LD), one of the most common vector-borne diseases in the Northern Hemisphere. Here, we solve the crystal structure of a mutated Bb vaccine antigen, CspZ-YA that lacks the ability to bind to host complement factor H (FH). We generate point mutants of CspZ-YA and identify CspZ-YAI183Y and CspZ-YAC187S to trigger more robust bactericidal responses. Compared to CspZ-YA, these CspZ-YA mutants require a lower immunization frequency to protect mice from LD-associated inflammation and bacterial colonization. Antigenicity of wild-type and mutant CspZ-YA proteins are similar, as measured using sera from infected people or immunized female mice. Structural comparison of CspZ-... More

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