Intracellular activity and in vivo efficacy in a mouse model of septic arthritis of the novel pseudopeptide Pep16 against Staphylococcus aureus clinical isolates.

IF 3.7 Q2 INFECTIOUS DISEASES JAC-Antimicrobial Resistance Pub Date : 2024-02-26 eCollection Date: 2024-02-01 DOI:10.1093/jacamr/dlae025
Jean-Baptiste Mascary, Valérie Bordeau, Irène Nicolas, Marie-Clémence Verdier, Pierre Rocheteau, Vincent Cattoir
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Abstract

Objectives: Assessing the therapeutic potential of a novel antimicrobial pseudopeptide, Pep16, both in vitro and in vivo for the treatment of septic arthritis caused by Staphylococcus aureus.

Methods: Seven clinical isolates of S. aureus (two MRSA and five MSSA) were studied. MICs of Pep16 and comparators (vancomycin, teicoplanin, daptomycin and levofloxacin) were determined through the broth microdilution method. The intracellular activity of Pep16 and levofloxacin was assessed in two models of infection using non-professional (osteoblasts MG-63) or professional (macrophages THP-1) phagocytic cells. A mouse model of septic arthritis was used to evaluate the in vivo efficacy of Pep16 and vancomycin. A preliminary pharmacokinetic (PK) analysis was performed by measuring plasma concentrations using LC-MS/MS following a single subcutaneous injection of Pep16 (10 mg/kg).

Results: MICs of Pep16 were consistently at 8 mg/L for all clinical isolates of S. aureus (2- to 32-fold higher to those of comparators) while MBC/MIC ratios confirmed its bactericidal activity. Both Pep16 and levofloxacin (when used at 2 × MIC) significantly reduced the bacterial load of all tested isolates (two MSSA and two MRSA) within both osteoblasts and macrophages. In MSSA-infected mice, Pep16 demonstrated a significant (∼10-fold) reduction on bacterial loads in knee joints. PK analysis following a single subcutaneous administration of Pep16 revealed a gradual increase in plasma concentrations, reaching a peak of 5.6 mg/L at 12 h.

Conclusions: Pep16 is a promising option for the treatment of septic arthritis due to S. aureus, particularly owing to its robust intracellular activity.

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新型假肽 Pep16 对抗金黄色葡萄球菌临床分离株的细胞内活性和在脓毒性关节炎小鼠模型中的体内疗效。
研究目的评估新型抗菌假肽 Pep16 在体外和体内治疗由金黄色葡萄球菌引起的化脓性关节炎的潜力:方法:研究了七种临床分离的金黄色葡萄球菌(两种 MRSA 和五种 MSSA)。通过肉汤微稀释法测定了 Pep16 和比较药(万古霉素、替考拉宁、达托霉素和左氧氟沙星)的 MICs。在两种感染模型中,使用非专业(成骨细胞 MG-63)或专业(巨噬细胞 THP-1)吞噬细胞评估了 Pep16 和左氧氟沙星的细胞内活性。小鼠脓毒性关节炎模型用于评估 Pep16 和万古霉素的体内疗效。通过使用 LC-MS/MS 测量单次皮下注射 Pep16(10 毫克/千克)后的血浆浓度,进行了初步的药代动力学(PK)分析:结果:对所有临床分离的金黄色葡萄球菌而言,Pep16 的 MIC 始终为 8 mg/L(比对比药高出 2 到 32 倍),而 MBC/MIC 比值证实了其杀菌活性。Pep16 和左氧氟沙星(在 MIC 值为 2 倍时使用)都能显著减少成骨细胞和巨噬细胞中所有受测分离菌(两种 MSSA 和两种 MRSA)的细菌负荷。在 MSSA 感染的小鼠中,Pep16 能显著减少膝关节中的细菌量(10 倍)。单次皮下注射 Pep16 后的 PK 分析显示,血浆浓度逐渐升高,12 小时后达到 5.6 mg/L 的峰值:结论:Pep16是治疗金黄色葡萄球菌引起的化脓性关节炎的一种很有前景的选择,特别是由于其强大的细胞内活性。
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CiteScore
5.30
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审稿时长
16 weeks
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