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Global priority multidrug-resistant pathogens do not resist photodynamic therapy

机译:全球优先级多药物抗性病原体不抵抗光动力疗法

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摘要

Microbial drug-resistance demands immediate implementation of novel therapeutic strategies. Antimicrobial photodynamic therapy (aPDT) combines the administration of a photosensitizer (PS) compound with low-irradiance light to induce photochemical reactions that yield reactive oxygen species (ROS). Since ROS react with nearly all biomolecules, aPDT offers a powerful multitarget method to avoid selection of drug-resistant strains. In this study, we assayed photodynamic inactivation under a standardized method, combining methylene blue (MB) as PS and red light, against global priority pathogens. The species tested include Acinetobacter baumannii, Klebsiella aerogenes, Escherichia coli, Klebsiella pneumoniae, Pseudomonas aeruginosa, Enterococcus faecium, Enterococcus faecalis, Staphylococcus aureus, Candida albicans and Cryptococcus neoformans. Our strain collection presents resistance to all tested antimicrobials ( > 50). All drug-resistant strains were compared to their drugsensitive counterparts. Regardless of resistance phenotype, MB-aPDT presented species-specific dose-response kinetics. More than 5log(10) reduction was observed within less than 75 s of illumination for A. baumannii, E. coli, E. faecium, E. faecalis and S. aureus and within less than 7 min for K. aerogenes, K. pneumoniae, P. aeruginosa, C. albicans and C. neoformans. No signs of correlations in between drug-resistance profiles and aPDT sensitivity were observed. Therefore, MB-aPDT can provide effective therapeutic protocols for a very broad spectrum of pathogens. Hence, we believe that this study represents a very important step to bring aPDT closer to implementation into mainstream medical practices.
机译:微生物耐药要求立即实施新的治疗策略。抗微生物光动力治疗(APDT)将光敏剂(PS)化合物与低辐照灯施用相结合,诱导产生反应性氧(ROS)的光化学反应。由于ROS与几乎所有的生物分子反应,APDT提供了一种强大的多元方法,以避免选择耐药菌株。在该研究中,我们在标准化方法下测定光动力灭活,将亚甲基蓝(MB)与PS和红光组合,反对全球优先级病原体。所测试的物种包括鲍曼氏菌,Klebsiella Aerogenes,大肠杆菌,Klebsiella肺炎,假单胞菌Aerginosa,肠球菌粪便,肠球菌粪,金黄色葡萄球菌,念珠菌白葡萄球菌,念珠菌蛋白质,念珠菌和水蛭肠炎群岛。我们的应变系列具有对所有测试的抗微生物(> 50)的抵抗力。将所有耐药菌株与其药物敏感对应物进行比较。无论抵抗表型如何,Mb-APDT呈现特异性剂量 - 反应动力学。在少于75岁以下的A.Baumannii,大肠杆菌,E. faecium,E. faecalis和S. aureus的少于75岁以下观察到超过5升(10)减少,并且在少于7分钟内,K. Aerogenes,K.Pneumoniae ,p. eruginosa,c. albicans和c. neoformans。没有观察到耐药型材和APDT敏感性之间的相关迹象。因此,MB-APDT可以为非常广泛的病原体提供有效的治疗方案。因此,我们认为这项研究代表了将APDT更接近实施的非常重要的一步,进入主流医疗实践。

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