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A synergistic anti-bacterial effect with cold atmospheric plasma (cap) and silver antibiotic nanoparticles

机译:与冷大气等离子体(帽)和抗生素银纳米颗粒的协同抗菌作用

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Introduction: As we all know, bacteria play a central role in the development of infections, and eradicating specific pathogenic bacteria without an adverse effect on normal mammalian cells still remains a major challenge in medicine today. Traditional anti-microbial applications involve antibiotics, UV photons, and/or nanoparticles, but they all have shortcomings such as the development of antibiotic-resistant bacteria and a low efficacy for killing specific bacteria. Cold-atmospheric plasma (CAP) is emphasized here as a novel effective alternative to traditional antibiotics for non-systemic infections due to the role plasma treatment may play against a range of microorganisms, even including antibiotic-resistant biofilm-forming strains and spores, with minimal damage to surrounding cells El. Materials and Methods: Here, methicillin (as a model antibiotic) and silver nanoparticles were encapsulated inside polymersomes by a self-assembly method. The encapsulated polymersomes were characterized for shape, chemistry, drug release and ultimately were then exposed to multidrug-resistant Escherichia coli at log phase prepared in fresh medium diluted to an optical density equivalent to 5~*106 CFU/ml. Aliquots from standardized bacterial suspension were additionally exposed to the cold plasma plume for various treatment times. After plasma exposure, each sample was transferred to fresh medium and a spectrophotometer was used to determine the speed of bacteria proliferation and shape of bacterial growth curves. All experiments were repeated in triplicate at least three times. Results and Discussion: This study showed that it is possible to overcome antibiotic-resistance through the presently combined delivery of silver nanoparticles and methicillin with the application of CAP. The antibacterial effect improved when polymersome concentration increased. The combined treatment of polymersomes and CAP resulted in a synergistic activity sufficient to delay or completely inhibit the growth of multidrug resistance bacteria. Under same concentration of polymersomes, bacterial growth was further delayed with CAP post-treatment when compared with non-CAP treatment. This was especially true for the all polymersome concentration where bacterial growth was delayed after 24 hrs, the longest time point studied here. Conclusions: The present study demonstrated that antibiotics and silver nanoparticles can be successfully encapsulated into polymersomes. Impressively, these polymersome nanoparticles combined with CPA therapy can significantly delay or completely inhibit the growth of multi-drug resistant bacteria.
机译:简介:众所周知,细菌在感染的发展中起着核心作用,而在不破坏正常哺乳动物细胞的不利影响的情况下根除特定的致病细菌仍然是当今医学的主要挑战。传统的抗微生物应用涉及抗生素,紫外线光子和/或纳米颗粒,但是它们都有缺点,例如发展了抗生素抗性细菌,并且杀死特定细菌的功效很低。由于血浆治疗可能对多种微生物(甚至包括具有抗生素抗性的生物膜形成菌株和孢子)发挥作用,因此,在非系统性感染方面,这里强调将冷大气血浆(CAP)作为传统抗生素的一种新型有效替代品。对周围细胞El的损害最小材料和方法:在这里,甲氧西林(作为模型抗生素)和银纳米颗粒通过自组装方法封装在多聚体中。对包封的聚合物小体的形状,化学性质,药物释放进行表征,然后最终将其在对数期暴露于对多药耐药的大肠杆菌中,该大肠杆菌在新鲜培养基中制备,稀释后的光密度等于5〜* 106 CFU / ml。将来自标准细菌悬浮液的等分试样另外暴露于冷血浆羽流中各种处理时间。暴露于血浆后,将每个样品转移到新鲜培养基中,并使用分光光度计确定细菌增殖的速度和细菌生长曲线的形状。所有实验一式三份重复至少三次。结果与讨论:这项研究表明,通过目前使用CAP的银纳米颗粒和甲氧西林的联合给药,可以克服抗生素耐药性。当多聚体的浓度增加时,抗菌效果得到改善。聚合体和CAP的联合处理产生了足以延迟或完全抑制耐多药细菌生长的协同活性。在相同浓度的聚合物囊泡中,与非CAP处理相比,CAP后处理可进一步延迟细菌的生长。对于所有多聚体浓度来说尤其如此,其中细菌生长在24小时后被延迟,这是这里研究的最长时间点。结论:本研究表明,抗生素和银纳米颗粒可以成功地封装到多聚体中。令人印象深刻的是,这些多聚体纳米颗粒与CPA治疗相结合可以显着延迟或完全抑制耐多药细菌的生长。

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