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噬菌体与抗生素联合治疗可预防野生型和上皮细胞感染。

Combined Bacteriophage and Antibiotic Treatment Prevents Infection of Wild Type and - Epithelial Cells.

作者信息

Luscher Alexandre, Simonin Juliette, Falconnet Léna, Valot Benoît, Hocquet Didier, Chanson Marc, Resch Grégory, Köhler Thilo, van Delden Christian

机构信息

Transplant Infectious Diseases Unit, Geneva University Hospitals, Geneva, Switzerland.

Department of Microbiology and Molecular Medicine, University of Geneva, Geneva, Switzerland.

出版信息

Front Microbiol. 2020 Aug 26;11:1947. doi: 10.3389/fmicb.2020.01947. eCollection 2020.

Abstract

With the increase of infections due to multidrug resistant bacterial pathogens and the shortage of antimicrobial molecules with novel targets, interest in bacteriophages as a therapeutic option has regained much attraction. Before the launch of future clinical trials, studies are required to better evaluate the efficacies and potential pitfalls of such therapies. Here we studied in an human airway epithelial cell line model the efficacy of phage and ciprofloxacin alone and in combination to treat infection by . The Calu-3 cell line and the isogenic CFTR knock down cell line (-) infected apically with strain PAO1 showed a progressive reduction in transepithelial resistance during 24 h. Administration at 6 h p.i. of single phage, phage cocktails or ciprofloxacin alone prevented epithelial layer destruction at 24 h p.i. Bacterial regrowth, due to phage resistant mutants harboring mutations in LPS synthesis genes, occurred thereafter both and . However, co-administration of two phages combined with ciprofloxacin efficiently prevented PAO1 regrowth and maintained epithelial cell integrity at 72 p.i. The phage/ciprofloxacin treatment did not induce an inflammatory response in the tested cell lines as determined by nanoString gene expression analysis. We conclude that combination of phage and ciprofloxacin efficiently protects wild type and - epithelial cells from infection by and emergence of phage resistant mutants without inducing an inflammatory response. Hence, phage-antibiotic combination should be a safe and promising anti-Pseudomonas therapy for future clinical trials potentially including cystic fibrosis patients.

摘要

随着多重耐药细菌病原体导致的感染增加以及新型靶点抗菌分子的短缺,噬菌体作为一种治疗选择重新引起了人们的极大关注。在开展未来的临床试验之前,需要进行研究以更好地评估此类疗法的疗效和潜在缺陷。在此,我们在人呼吸道上皮细胞系模型中研究了单独使用噬菌体和环丙沙星以及两者联合使用治疗由[病原体名称未给出]引起的感染的疗效。用PAO1菌株顶端感染Calu - 3细胞系和同基因CFTR敲低细胞系(-)后,在24小时内跨上皮电阻逐渐降低。在感染后6小时给予单一噬菌体、噬菌体鸡尾酒或单独的环丙沙星可防止在感染后24小时上皮层破坏。此后,由于在LPS合成基因中携带突变的噬菌体抗性突变体,[两种细胞系均出现]细菌再生长。然而,两种噬菌体与环丙沙星联合给药可有效防止PAO1再生长,并在感染后72小时维持上皮细胞完整性。通过nanoString基因表达分析确定,噬菌体/环丙沙星治疗在受试细胞系中未诱导炎症反应。我们得出结论,噬菌体和环丙沙星联合使用可有效保护野生型和[CFTR敲低]上皮细胞免受[病原体名称未给出]感染以及噬菌体抗性突变体的出现,且不诱导炎症反应。因此,噬菌体 - 抗生素联合使用对于未来可能包括囊性纤维化患者的临床试验应该是一种安全且有前景的抗铜绿假单胞菌疗法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fb0d/7479825/d0bb5ea4f19f/fmicb-11-01947-g001.jpg

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