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MnTE-2-PyP在一种新型骨折模型中破坏金黄色葡萄球菌生物膜。

MnTE-2-PyP disrupts Staphylococcus aureus biofilms in a novel fracture model.

作者信息

Lindsay Sarah E, Lindsay Hunter G, Kallet Julia, Weaver Michael R, Curran-Everett Douglas, Crapo James D, Regan Elizabeth A

机构信息

National Jewish Health, Denver, Colorado, USA.

出版信息

J Orthop Res. 2021 Nov;39(11):2439-2445. doi: 10.1002/jor.24967. Epub 2021 Jan 2.

DOI:10.1002/jor.24967
PMID:33347639
Abstract

Biofilm-associated infections in orthopedic surgery lead to worse clinical outcomes and greater morbidity and mortality. The scope of the problem encompasses infected total joints, internally fixed fractures, and implanted devices. Diagnosis is difficult. Cultures are often negative, and antibiotic treatments are ineffective. The infections resist killing by the immune system and antibiotics. The organized matrix structure of extracellular polymeric substances within the biofilm shields and protects the bacteria from identification and immune cell action. Bacteria in biofilms actively modulate their redox environment and can enhance the matrix structure by creating an oxidizing environment. We postulated that a potent redox-active metalloporphyrin MnTE-2-PyP (chemical name: manganese (II) meso-tetrakis-(N-methylpyridinium-2-yl) porphyrin) that scavenges reactive species and modulates the redox state to a reduced state, would improve the effect of antibiotic treatment for a biofilm-associated infection. An infected fracture model with a midshaft femoral osteotomy was created in C57B6 mice, internally fixed with an intramedullary 23-gauge needle and seeded with a biofilm-forming variant of Staphylococcus aureus. Animals were divided into three treatment groups: control, antibiotic alone, and combined antibioticplus MnTE-2-PyP. The combined treatment group had significantly decreased bacterial counts in harvested bone, compared with antibiotic alone. In vitro crystal violet assay of biofilm structure and corresponding nitroblue tetrazolium assay for reactive oxygen species (ROS) demonstrated that MnTE-2-PyP decreased the biofilm structure and reduced ROS in a correlated and dose-dependent manner. The biofilm structure is redox-sensitive in S. aureus and an ROS scavenger improved the effect of antibiotic therapy in model of biofilm-associated infections.

摘要

骨科手术中与生物膜相关的感染会导致更差的临床结果以及更高的发病率和死亡率。问题范围包括感染的全关节、内固定骨折和植入装置。诊断困难。培养结果往往为阴性,抗生素治疗无效。这些感染能抵抗免疫系统和抗生素的杀灭作用。生物膜内细胞外聚合物的有序基质结构可保护细菌,使其不被识别且免受免疫细胞作用。生物膜中的细菌会主动调节其氧化还原环境,并通过创造氧化环境来增强基质结构。我们推测,一种强效的氧化还原活性金属卟啉MnTE-2-PyP(化学名称:锰(II)中-四(N-甲基吡啶-2-基)卟啉),它能清除活性物质并将氧化还原状态调节至还原态,会提高抗生素治疗生物膜相关感染的效果。在C57B6小鼠中建立了中段股骨干截骨的感染性骨折模型,用23号髓内针进行内固定,并接种金黄色葡萄球菌的生物膜形成变体。动物被分为三个治疗组:对照组、单独使用抗生素组和抗生素加MnTE-2-PyP联合治疗组。与单独使用抗生素组相比,联合治疗组收获的骨组织中细菌数量显著减少。生物膜结构的体外结晶紫测定以及相应的活性氧(ROS)硝基蓝四唑测定表明,MnTE-2-PyP以相关且剂量依赖的方式减少了生物膜结构并降低了ROS。金黄色葡萄球菌中的生物膜结构对氧化还原敏感,一种ROS清除剂改善了生物膜相关感染模型中抗生素治疗的效果。

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