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Carbene formation as a mechanism for efficient intracellular uptake of cationic antimicrobial carbon acid polymers

Author(s)
Koh, Chong Hui; Lambu, Mallikharjuna Rao; Tan, Chongyun; Wei, Guangmin; Kok, Zhi Yuan; Zhang, Kaixi; Vu, Quang Huy Nhat; Panneerselvam, Muthuvel; Ooi, Ying Jie; Tan, Shiow Han; Wang, Zheng; Tatina, Madhu Babu; Ng, Justin Tze Yang; Guo, Aoxin; Tonanon, Panyawut; Dang, Tram T; Gan, Yunn-Hwen; Mu, Yuguang; Hammond, Paula T; Chi, Yonggui Robin; Webster, Richard D; Pullarkat, Sumod A; Li, Qingjie; Greenberg, E Peter; Gründling, Angelika; Pethe, Kevin; Chan-Park, Mary B; ... Show more Show less
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Abstract
Cationic polymers have emerged as promising next-generation antimicrobial agents, albeit with inherent limitations such as low potency and limited biocompatibility. Classical cationic polymers kill bacteria via physical membrane disruption. We propose a non-classical mechanism of crossing the bacterial plasma membrane barrier, a step required for subsequent inhibition of intracellular targets, by cationic polymers which are carbon acids. Oligoimidazolium (OIM) carbon acids, instead of lysing bacteria, transiently deprotonate in water to form hydrophobic N-heterocyclic carbenes (NHCs) and exhibit efficient plasma membrane translocation. Only OIMs that are carbon acids have potent antibacterial activities against even colistin- and multidrug-resistant bacteria. OIM amide derivatives exhibit excellent antibacterial efficacy in murine sepsis and thigh infection models, while a polymeric version acts as a prophylactic agent against bovine mastitis, which is a global agricultural problem. This study unveils a promising path for the development of an alternative class of potent antimicrobial agents.
Date issued
2025-07-12
URI
https://hdl.handle.net/1721.1/160555
Department
Massachusetts Institute of Technology. Department of Chemical Engineering
Journal
Nature Communications
Publisher
Springer Science and Business Media LLC
Citation
Koh, C.H., Lambu, M.R., Tan, C. et al. Carbene formation as a mechanism for efficient intracellular uptake of cationic antimicrobial carbon acid polymers. Nat Commun 16, 6460 (2025).
Version: Final published version

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