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Influence of cationic groups on the antibacterial behavior of cationic nano-sized hyperbranched polymers to enhance bacteria-infected wound healing

机译:阳离子基团对阳离子纳米超支化聚合物抗菌行为的影响,促进细菌感染创面愈合

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摘要

With the continuous emergence of drug-resistant pathogens, new strategies with high antibacterial efficacy are urgently needed. Herein, five cationic nano-sized hyperbranched polymers (CNHBPs) with cationic functional groups have been constructed, and their antibacterial mechanism has been studied in detail. CNHBPs bearing secondary ammonium salt groups and long alkyl chains (S12-CNHBP) exhibited weak antibacterial and antibiofilm ability, while CNHBPs bearing quaternary ammonium salt groups and long alkyl chains (Q12-CNHBP) showed the highest antimicrobial and strongest antibiofilm activities. ζ potential and isothermal titration microcalorimetry (ITC) results suggest that the negatively charged surfaces of bacterial cells provided Q12-CNHBP with a higher intrinsic electrostatic driving force for bacterial killing than that with S12-CNHBP. Fluorescent tracing and morphological observations indicate that the bacterial genome might be another antibacterial target for S12-CNHBP in addition to the cell wall and membrane, which are mainly antibacterial targets for Q12-CNHBP, making it less likely to induce bacterial resistance. Surprisingly, Q12-CNHBP exhibited superior in vivo therapeutic efficacy in a mouse wound model of methicillin-resistant Staphylococcus aureus (MRSA) infection with low toxicity during treatment. These advantages and ease of preparation will undoubtedly distinguish Q12-CNHBP as a new class of suitable candidates to combat multidrug-resistant pathogen infections. This study opens up a new avenue for exploiting antibacterial biomaterials to treat infections caused by drug-resistant bacteria.
机译:连续出现耐药性病原体,与高抗菌新策略功效是急需的。阳离子纳米级的超支化聚合物(CNHBPs)与阳离子基团被建造,抗菌详细机理进行了研究。轴承二级铵盐组和长烷基链(S12-CNHBP)表现出弱抗菌和antibiofilm能力,CNHBPs轴承季铵盐组和烷基长链(Q12-CNHBP)显示最高的抗菌和antibiofilm最强活动。结果表明,微量热法(ITC)带负电荷的细菌细胞的表面Q12-CNHBP提供了一个更高的内在静电驱动力的细菌杀死与S12-CNHBP比。形态学观察表明,细菌基因组可能是另一个抗菌目标S12-CNHBP除了细胞壁和膜主要抗菌Q12-CNHBP目标,使得它不太可能诱导细菌耐药性。Q12-CNHBP表现出优越的体内治疗老鼠伤口模型的有效性耐甲氧西林金黄色葡萄球菌(MRSA)感染中毒性较低治疗。准备无疑将区分Q12-CNHBP作为一类新的合适的候选人应对耐多药病原体感染。利用抗菌生物材料来治疗耐药细菌引起的感染。

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