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噬菌体治疗产 CTX-M-15 型大肠埃希菌 O25b:H4-ST131 克隆引起的实验性脓毒症和脑膜炎的疗效。

Efficacy of bacteriophage therapy in experimental sepsis and meningitis caused by a clone O25b:H4-ST131 Escherichia coli strain producing CTX-M-15.

机构信息

Université Paris Diderot, Sorbonne Paris Cité, Equipe d'Accueil EA3105, and AP-HP, Hôpital Robert Debré, Paris, France.

出版信息

Antimicrob Agents Chemother. 2012 Jul;56(7):3568-75. doi: 10.1128/AAC.06330-11. Epub 2012 Apr 9.

Abstract

We evaluated phage therapy in experimental infections due to S242, a fatal neonatal meningitis Escherichia coli strain belonging to the worldwide-distributed O25b:H4-ST131 clone that produces extended-spectrum beta-lactamase CTX-M-15. A lytic phage, EC200(PP), active against S242, was isolated from environmental water. After determining in vitro and ex vivo stabilities and pharmacokinetic properties of EC200(PP) in rat pups, we assessed the therapeutic efficacy of a single dose of 10(8) PFU using models of sepsis and meningitis in which fatality was 100%. EC200(PP) was partially neutralized by human serum. In contrast to the high concentration of phage in the spleen and the kidney, low titers in urine and the central nervous system were observed. Nevertheless, in the sepsis model, EC200(PP) administered 7 h or 24 h postinfection resulted in 100% and 50% pup survival, respectively. In the meningitis model, EC200(PP) administered 1 h or 7 h postinfection rescued 100% of the animals. The most delayed treatments were associated with the selection of phage-resistant S242 mutants. However, a representative mutant was highly sensitive to killing serum activity and avirulent in an animal model. EC200(PP) is a potential therapeutic agent for sepsis and meningitis caused by the widespread E. coli O25:H4-ST131 multidrug-resistant clone.

摘要

我们评估了噬菌体疗法在 S242 引起的实验性感染中的效果,S242 是一种致命的新生儿脑膜炎大肠杆菌菌株,属于广泛分布的 O25b:H4-ST131 克隆,能产生扩展谱β-内酰胺酶 CTX-M-15。从环境水中分离到了一种对 S242 有裂解作用的噬菌体 EC200(PP)。在确定了 EC200(PP)在大鼠幼仔体内的体外和离体稳定性以及药代动力学特性后,我们评估了单次给予 10(8)PFU 的治疗效果,采用了败血症和脑膜炎模型,其中死亡率为 100%。EC200(PP)部分被人血清中和。与脾和肾中噬菌体的高浓度相比,尿液和中枢神经系统中的滴度较低。尽管如此,在败血症模型中,EC200(PP)在感染后 7 小时或 24 小时给药,分别导致 100%和 50%的幼仔存活。在脑膜炎模型中,EC200(PP)在感染后 1 小时或 7 小时给药可挽救 100%的动物。最延迟的治疗与噬菌体耐药 S242 突变体的选择有关。然而,一个代表性的突变体对杀菌血清活性高度敏感,在动物模型中无毒力。EC200(PP)是一种针对广泛存在的大肠杆菌 O25:H4-ST131 多药耐药克隆引起的败血症和脑膜炎的潜在治疗剂。

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