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Romo1-Derived Antimicrobial Peptide Is a New Antimicrobial Agent against Multidrug-Resistant Bacteria in a Murine Model of Sepsis

机译:Romo1衍生的抗菌肽是一种新的抗微生物剂,用于败血症的小鼠模型中的多药抗性细菌

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To overcome increasing bacterial resistance to conventional antibiotics, many antimicrobial peptides (AMPs) derived from host defense proteins have been developed. However, there are considerable obstacles to their application to systemic infections because of their low bioavailability. In the present study, we developed an AMP derived from Romo1 (AMPR-11) that exhibits a broad spectrum of antimicrobial activity. AMPR-11 showed remarkable efficacy against sepsis-causing bacteria, including multidrug-resistant strains, with low toxicity in a murine model of sepsis after intravenous administration. It seems that AMPR-11 disrupts bacterial membranes by interacting with cardiolipin and lipid A. From the results of this study, we suggest that AMPR-11 is a new class of agent for overcoming low efficacy in the intravenous application of AMPs and is a promising candidate to overcome multidrug resistance.
机译:为了克服对常规抗生素的增加,已经开发出源自宿主防蛋白的许多抗微生物肽(AMPs)。然而,由于生物利用度低,它们对系统性感染的应用具有相当大的障碍。在本研究中,我们开发了衍生自ROMO1(AMPR-11)的放大器,其具有广泛的抗微生物活性。 AMPR-11显示出对脓毒症引起的细菌的显着疗效,包括多药抗菌菌株,在静脉内给药后脓毒症的小鼠模型中具有低毒性。似乎AMPR-11通过与心肌脂和脂A相互作用来破坏细菌膜。从本研究的结果中,我们建议AMPR-11是克服安培静脉内施用低疗效的新类药剂,并且是一个有前途的克服多药抗性的候选者。

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