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首页> 外文期刊>The Journal of Infectious Diseases >Bacteriophage-Loaded Nanostructured Lipid Carrier: Improved Pharmacokinetics Mediates Effective Resolution of Klebsiella pneumoniae-Induced Lobar Pneumonia
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Bacteriophage-Loaded Nanostructured Lipid Carrier: Improved Pharmacokinetics Mediates Effective Resolution of Klebsiella pneumoniae-Induced Lobar Pneumonia

机译:噬菌体负载的纳米脂质载体:改进的药代动力学可以有效解决肺炎克雷伯菌引起的大叶性肺炎

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摘要

This study examined the therapeutic and prophylactic potential of bacteriophages in a mouse model of Klebsiella pneumoniae lobar pneumonia. Phages were administered intraperitoneally. Liposome-entrapped phages (LP) were effective in treating infection, even when therapy was delayed by 3 days after the induction of pneumonia. In contrast, nonliposomal phages provided protection when administered 24 hours after infection. Administration of nonliposomal phages 6 hours prior to intranasal bacterial challenge resulted in complete protection, compared with LP, which was effective even when administered 48 hours prior to infection. Increased reduction and a greater increment in the levels of proinflammatory and antiinflammatory cytokines, respectively, in homogenates of lung from LP-treated mice were suggestive of increased efficacy of LP in the treatment of pneumonia. This is the first study to assess liposomes as a delivery vehicle for phage, and the results confirm the superiority of LP for both therapeutic and prophylactic applications.
机译:这项研究检查了噬菌体在肺炎克雷伯菌肺叶性肺炎小鼠模型中的治疗和预防潜力。腹膜内给予噬菌体。包裹脂质体的噬菌体(LP)可有效治疗感染,即使在诱发肺炎后将治疗推迟了3天也是如此。相反,非脂质体噬菌体在感染后24小时给药时可提供保护。与LP相比,在鼻内细菌攻击前6小时施用非脂质体噬菌体可实现完全保护,即使在感染前48小时施用也有效。 LP处理小鼠的肺匀浆中分别减少的减少和促炎和抗炎细胞因子水平的增加更大,表明LP治疗肺炎的功效增加。这是第一项评估脂质体作为噬菌体递送载体的研究,结果证实了LP在治疗和预防应用方面的优越性。

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