Antibiotic-Polymer Self-Assembled Nanocomplex to Reverse Phenotypic Resistance of Bacteria toward Last-Resort Antibiotic Colistin.
Huimin ZhaoLan-Lan ZhongChuan YangNing TangYanwei HeWan HeZihan ZhaoChangbu WuPeiyan YuanYi Yan YangGuo-Bao TianXin DingPublished in: ACS nano (2023)
Colistin is the last-resort antibiotic to treat multidrug-resistant (MDR) Gram-negative bacterial infections that are untreatable by other clinically available antibiotics. However, the recently merged plasmid-borne gene mobilized colistin resistance ( mcr ) leads to modification of the colistin target (i.e., bacterial membrane), greatly compromising the therapy outcome of colistin. To address this unmet clinical need, a nanocomplex (CMS-pEt_20 NP) of anionic prodrug colistin methanesulfonate (CMS) and guanidinium-functionalized cationic polymer pEt_20 is developed through facile self-assembly for co-delivering an antibiotic and antimicrobial polymer with membrane affinity to reverse colistin resistance. The CMS-pEt_20 NP formation enables reversal of colistin resistance and complete killing of clinically isolated mcr -positive colistin-resistant bacteria including MDR E. coli and K. pneumoniae , while monotreatment of polymer or antibiotic at equivalent doses exhibits no antibacterial activity. Mechanistic studies reveal that the CMS-pEt_20 NP enhanced the affinity of delivered CMS to the modified membrane of colistin-resistant bacteria, reviving the membrane lytic property of colistin. The increased membrane permeability caused by colistin in turn promotes an influx of pEt_20 to generate intracellular ROS stress, resulting in elimination of colistin-resistant bacteria. More importantly, a colistin-resistant mouse peritonitis-sepsis infection model demonstrates the excellent therapeutic efficacy of CMS-pEt_20 NP with 100% survival of the infected mouse. In addition, the nanocomplex is proven not toxic both in vitro and in vivo . Taken together, the self-assembled antibiotic-polymer nanocomplex with two complementary antibacterial mechanisms successfully reverses the colistin resistance phenotype in bacteria, and it can be a potential strategy to treat untreatable colistin-resistant MDR bacterial infections.
Keyphrases
- multidrug resistant
- gram negative
- acinetobacter baumannii
- escherichia coli
- klebsiella pneumoniae
- drug resistant
- pseudomonas aeruginosa
- pet ct
- pet imaging
- staphylococcus aureus
- genome wide
- cystic fibrosis
- gene expression
- gold nanoparticles
- climate change
- crispr cas
- dna methylation
- heat stress
- highly efficient
- oxidative stress
- liquid chromatography
- single cell
- sensitive detection
- capillary electrophoresis