Author
Listed:
- Kaixi Zhang
(Nanyang Technological University
Nanyang Technological University)
- Yu Du
(Nanyang Technological University
Nanyang Technological University
Chinese Academy of Sciences)
- Zhangyong Si
(Nanyang Technological University
Nanyang Technological University)
- Yang Liu
(Nanyang Technological University
Nanyang Technological University)
- Michelle E. Turvey
(Singapore-MIT Alliance for Research & Technology Centre)
- Cheerlavancha Raju
(Nanyang Technological University
Nanyang Technological University)
- Damien Keogh
(Nanyang Technological University
Nanyang Technological University)
- Lin Ruan
(Nanyang Technological University
Nanyang Technological University)
- Subramanion L. Jothy
(Nanyang Technological University
Nanyang Technological University)
- Sheethal Reghu
(Nanyang Technological University
Nanyang Technological University)
- Kalisvar Marimuthu
(Tan Tock Seng Hospital
National Centre for Infectious Diseases)
- Partha Pratim De
(Tan Tock Seng Hospital)
- Oon Tek Ng
(Tan Tock Seng Hospital
National Centre for Infectious Diseases
Nanyang Technological University)
- José R. Mediavilla
(Hackensack Meridian Health)
- Barry N. Kreiswirth
(Hackensack Meridian Health)
- Yonggui Robin Chi
(Nanyang Technological University)
- Jinghua Ren
(Huazhong University of Science & Technology)
- Kam C. Tam
(University of Waterloo)
- Xue-Wei Liu
(Nanyang Technological University
Nanyang Technological University)
- Hongwei Duan
(Nanyang Technological University
Nanyang Technological University)
- Yabin Zhu
(Medical School of Ningbo University, Ningbo)
- Yuguang Mu
(Nanyang Technological University)
- Paula T. Hammond
(Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Guillermo C. Bazan
(University of California Santa Barbara)
- Kevin Pethe
(Nanyang Technological University
Nanyang Technological University
Nanyang Technological University)
- Mary B. Chan-Park
(Nanyang Technological University
Nanyang Technological University
Nanyang Technological University)
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.
Suggested Citation
Kaixi Zhang & Yu Du & Zhangyong Si & Yang Liu & Michelle E. Turvey & Cheerlavancha Raju & Damien Keogh & Lin Ruan & Subramanion L. Jothy & Sheethal Reghu & Kalisvar Marimuthu & Partha Pratim De & Oon , 2019.
"Enantiomeric glycosylated cationic block co-beta-peptides eradicate Staphylococcus aureus biofilms and antibiotic-tolerant persisters,"
Nature Communications, Nature, vol. 10(1), pages 1-14, December.
Handle:
RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-12702-8
DOI: 10.1038/s41467-019-12702-8
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