Targeting microbial biofilms: current and prospective therapeutic strategies

被引:0
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作者
Hyun Koo
Raymond N. Allan
Robert P. Howlin
Paul Stoodley
Luanne Hall-Stoodley
机构
[1] Biofilm Research Laboratories,Department of Orthodontics and Divisions of Pediatric Dentistry & Community Oral Health
[2] Levy Center for Oral Health,Department of Microbial Infection and Immunity
[3] School of Dental Medicine,Departments of Orthopaedics and Microbiology
[4] University of Pennsylvania,undefined
[5] Clinical and Experimental Sciences,undefined
[6] Faculty of Medicine and Institute for Life Sciences,undefined
[7] University of Southampton,undefined
[8] Southampton NIHR Wellcome Trust Clinical Research Facility,undefined
[9] University Hospital Southampton NHS Foundation Trust,undefined
[10] Centre for Biological Sciences,undefined
[11] University of Southampton,undefined
[12] Southampton NIHR Respiratory Biomedical Research Unit,undefined
[13] University Hospital Southampton NHS Foundation Trust,undefined
[14] Centre for Microbial Interface Biology,undefined
[15] The Ohio State University,undefined
[16] The Ohio State University,undefined
[17] National Centre for Advanced Tribology at Southampton (nCATS),undefined
[18] Faculty of Engineering and the Environment,undefined
[19] University of Southampton,undefined
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摘要
Biofilms harbour complex structural and biological attributes, such as the presence of an extracellular polymeric matrix, physical and chemical heterogeneity and drug tolerance, which provide remarkable therapeutic challenges.Biofilm drug tolerance is a consequence of complex physicochemical and biological properties with multiple microbial genetic and molecular factors, often involving polymicrobial interactions.The challenges to existing antimicrobial or monotherapeutic approaches by the multifactorial nature of biofilm development, combined with drug tolerance, requires robust effective multitargeted or combinatorial therapies.Combinatorial strategies are needed to eliminate existing biofilms by targeting vital structural and functional traits of biofilms, such as the EPS matrix and dormant cells, as well as approaches exploiting host–pathogen interactions.Promising technologies based on 'smart release' or 'on-demand activation' of bioactive agents when triggered by biofilm-derived cues can degrade the matrix and kill resident bacteria, and have the potential to eradicate the pathogenic niche with precision and minimal cytotoxicity to surrounding tissues.Validation of proof-of-concept studies using clinically relevant animal models, as well as clinical trials, are needed for rigorous evaluation.
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页码:740 / 755
页数:15
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