Enantiomeric glycosylated cationic block co-beta-peptides eradicate Staphylococcus aureus biofilms and antibiotic-tolerant persisters

Author:

Zhang Kaixi,Du YuORCID,Si Zhangyong,Liu Yang,Turvey Michelle E.,Raju Cheerlavancha,Keogh Damien,Ruan Lin,Jothy Subramanion L.,Reghu Sheethal,Marimuthu Kalisvar,De Partha Pratim,Ng Oon Tek,Mediavilla José R.,Kreiswirth Barry N.,Chi Yonggui Robin,Ren Jinghua,Tam Kam C.,Liu Xue-Wei,Duan HongweiORCID,Zhu Yabin,Mu YuguangORCID,Hammond Paula T.ORCID,Bazan Guillermo C.ORCID,Pethe Kevin,Chan-Park Mary B.ORCID

Abstract

Abstract The treatment of bacterial infections is hindered by the presence of biofilms and metabolically inactive persisters. Here, we report the synthesis of an enantiomeric block co-beta-peptide, poly(amido-D-glucose)-block-poly(beta-L-lysine), with high yield and purity by one-shot one-pot anionic-ring opening (co)polymerization. The co-beta-peptide is bactericidal against methicillin-resistant Staphylococcus aureus (MRSA), including replicating, biofilm and persister bacterial cells, and also disperses biofilm biomass. It is active towards community-acquired and hospital-associated MRSA strains which are resistant to multiple drugs including vancomycin and daptomycin. Its antibacterial activity is superior to that of vancomycin in MRSA mouse and human ex vivo skin infection models, with no acute in vivo toxicity in repeated dosing in mice at above therapeutic levels. The copolymer displays bacteria-activated surfactant-like properties, resulting from contact with the bacterial envelope. Our results indicate that this class of non-toxic molecule, effective against different bacterial sub-populations, has promising potential for the treatment of S. aureus infections.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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