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High prevalence of mgrB-mediated colistin resistance among carbapenem-resistant Klebsiella pneumoniae is associated with biofilm formation, and can be overcome by colistin-EDTA combination therapy
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AbstractThe global prevalence of colistin-resistant Klebsiella pneumoniae (ColRkp) facilitated by chromosomal and plasmid-mediated Ara4N or PEtN-remodeled LPS alterations has steadily increased with increased colistin usage for treating carbapenem-resistant K. pneumoniae (CRkp). Our study demonstrated the rising trend of ColRkp showing extensively and pandrug-resistant characteristics among CRkp, with a prevalence of 28.5%, which was mediated by chromosomal mgrB, pmrB, or phoQ mutations (91.5%), and plasmid-mediated mcr-1.1, mcr-8.1, mcr-8.2 alone or in conjunction with R256G PmrB (8.5%). Several genetic alterations in mgrB (85.1%) with increased expressions of Ara4N-related phoPQ and pmrK were critical for establishing colistin resistance in our isolates. In this study, we discovered the significant associations between extensively drug-resistant bacteria (XDR) and pandrug-resistant bacteria (PDR) ColRkp in terms of moderate, weak or no biofilm-producing abilities, and altered expressions of virulence factors. These ColRkp would therefore be very challenging to treat, emphasizing for innovative therapy to combat these infections. Regardless of the underlying colistin-resistant mechanisms, colistin-EDTA combination therapy in this study produced potent synergistic effects in both in vitro and in vivo murine bacteremia, with no ColRkp regrowth and improved animal survival, implying the significance of colistin-EDTA combination therapy as systemic therapy for unlocking colistin resistance in ColRkp-associated bacteremia.
Springer Science and Business Media LLC
Aye Mya Sithu Shein
Dhammika Leshan Wannigama
Paul G. Higgins
Cameron Hurst
Shuichi Abe
Parichart Hongsing
Naphat Chantaravisoot
Thammakorn Saethang
Sirirat Luk-in
Tingting Liao
Sumanee Nilgate
Ubolrat Rirerm
Naris Kueakulpattana
Sukrit Srisakul
Apichaya Aryukarn
Matchima Laowansiri
Lee Yin Hao
Manta Yonpiam
Naveen Kumar Devanga Ragupathi
Teerasit Techawiwattanaboon
Natharin Ngamwongsatit
Mohan Amarasiri
Puey Ounjai
Rosalyn Kupwiwat
Phatthranit Phattharapornjaroen
Vishnu Nayak Badavath
Asada Leelahavanichkul
Anthony Kicic
Tanittha Chatsuwan
Title: High prevalence of mgrB-mediated colistin resistance among carbapenem-resistant Klebsiella pneumoniae is associated with biofilm formation, and can be overcome by colistin-EDTA combination therapy
Description:
AbstractThe global prevalence of colistin-resistant Klebsiella pneumoniae (ColRkp) facilitated by chromosomal and plasmid-mediated Ara4N or PEtN-remodeled LPS alterations has steadily increased with increased colistin usage for treating carbapenem-resistant K.
pneumoniae (CRkp).
Our study demonstrated the rising trend of ColRkp showing extensively and pandrug-resistant characteristics among CRkp, with a prevalence of 28.
5%, which was mediated by chromosomal mgrB, pmrB, or phoQ mutations (91.
5%), and plasmid-mediated mcr-1.
1, mcr-8.
1, mcr-8.
2 alone or in conjunction with R256G PmrB (8.
5%).
Several genetic alterations in mgrB (85.
1%) with increased expressions of Ara4N-related phoPQ and pmrK were critical for establishing colistin resistance in our isolates.
In this study, we discovered the significant associations between extensively drug-resistant bacteria (XDR) and pandrug-resistant bacteria (PDR) ColRkp in terms of moderate, weak or no biofilm-producing abilities, and altered expressions of virulence factors.
These ColRkp would therefore be very challenging to treat, emphasizing for innovative therapy to combat these infections.
Regardless of the underlying colistin-resistant mechanisms, colistin-EDTA combination therapy in this study produced potent synergistic effects in both in vitro and in vivo murine bacteremia, with no ColRkp regrowth and improved animal survival, implying the significance of colistin-EDTA combination therapy as systemic therapy for unlocking colistin resistance in ColRkp-associated bacteremia.
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