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Structure-based redesign of lysostaphin yields potent antistaphylococcal enzymes that evade immune cell surveillance.

Mol Ther Methods Clin Dev. 2015; 
BlazanovicKristina,ZhaoHongliang,ChoiYoonjoo,LiWen,SalvatRegina S,OsipovitchDaniel C,FieldsJennifer,MoiseLeonard,BerwinBrent L,FieringSteven N,Bailey-KelloggChris,GriswoldKa
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Peptide Synthesis Peptides derived from the LST catalytic domain were ordered from GenScript (Piscataway, NJ) Get A Quote

摘要

Staphylococcus aureus infections exert a tremendous burden on the health-care system, and the threat of drug-resistant strains continues to grow. The bacteriolytic enzyme lysostaphin is a potent antistaphylococcal agent with proven efficacy against both drug-sensitive and drug-resistant strains; however, the enzyme's own bacterial origins cause undesirable immunogenicity and pose a barrier to clinical translation. Here, we deimmunized lysostaphin using a computationally guided process that optimizes sets of mutations to delete immunogenic T cell epitopes without disrupting protein function. In vitro analyses showed the methods to be both efficient and effective, producing seven different deimmunized des... More

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