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雾化利福昔明对比妥布霉素治疗铜绿假单胞菌肺炎小鼠的疗效。

Efficacy of Aerosolized Rifaximin versus Tobramycin for Treatment of Pseudomonas aeruginosa Pneumonia in Mice.

机构信息

Department of Biomedical Sciences, Joan C. Edwards School of Medicine at Marshall University, Huntington, West Virginia, USA.

Progenesis Technologies, LLC, Robert C. Byrd Biotechnology Science Center, Huntington, West Virginia, USA.

出版信息

Antimicrob Agents Chemother. 2019 Jun 24;63(7). doi: 10.1128/AAC.02341-18. Print 2019 Jul.

Abstract

is a Gram-negative opportunistic bacterial pathogen that can cause chronic lung infections in patients with cystic fibrosis (CF). The current preferred treatment for CF lung infections includes inhaled tobramycin (TOB); however, studies suggest TOB cannot effectively inhibit biofilm formation. Using an NIH small compounds drug library approved for safe use in humans, we identified rifaximin (RFX), a semisynthetic, rifamycin family, nonsystemic antibiotic that inhibits alginate production and growth in Inhibition of alginate production was further analyzed using the uronic acid carbazole assay and a promoter reporter assay that measures the transcription of the alginate biosynthetic operon. Compared to TOB, RFX significantly reduced alginate production in laboratory and CF sputum isolates of In addition, RFX showed a narrow range of MICs when measured with multidrug-resistant bacterial species of clinical relevance, synergistic activities with TOB or amikacin against clinical isolates, as well as reduction toward preformed biofilms. In C57BL/6 mice, penetration of nebulized TOB into the lungs was shown at a higher level than that of RFX. Further, assessment using a DBA/2 mouse lung infection model found increased survival rates with a single-dose treatment of nebulized RFX and decreased PAO1 bioburden with a multiple-dose treatment of RFX plus TOB. In addition, mice treated with a single exposure to dimethyl sulfoxide (DMSO), a solvent that dissolves RFX, showed no apparent toxicity. In summary, RFX may be used to supplement TOB inhalation therapy to increase efficacy against biofilm infections.

摘要

铜绿假单胞菌是一种革兰氏阴性机会性病原体,可导致囊性纤维化(CF)患者的慢性肺部感染。目前 CF 肺部感染的首选治疗方法包括吸入妥布霉素(TOB);然而,研究表明 TOB 不能有效抑制生物膜的形成。我们使用美国国立卫生研究院(NIH)批准的用于人类安全使用的小型化合物药物库,鉴定出利福昔明(RFX),一种半合成利福霉素家族的非系统性抗生素,可抑制海藻酸盐的产生和 利用糖醛酸咔唑测定法和测量藻酸盐生物合成操纵子转录的启动子报告测定法进一步分析了海藻酸盐产生的抑制作用。与 TOB 相比,RFX 显著降低了实验室和 CF 痰分离株中 此外,当用具有临床相关性的多药耐药细菌物种测量时,RFX 的 MIC 范围较窄,与 TOB 或阿米卡星具有协同活性,并且对 预先形成的生物膜也有减少作用。在 C57BL/6 小鼠中,雾化 TOB 进入肺部的穿透水平高于 RFX。此外,使用 DBA/2 小鼠肺部感染模型进行评估发现,雾化 RFX 单次治疗的存活率提高,雾化 RFX 加 TOB 多次治疗可降低 PAO1 生物负荷。此外,用溶解 RFX 的二甲亚砜(DMSO)溶剂单次处理的小鼠未显示出明显的毒性。总之,RFX 可用于补充 TOB 吸入治疗以提高针对 生物膜感染的疗效。

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