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抗病毒耐药性和噬菌体对抗生素耐药的肠外致病性细菌的反适应

Antiviral Resistance and Phage Counter Adaptation to Antibiotic-Resistant Extraintestinal Pathogenic .

机构信息

Department of Integrative Molecular and Biomedical Science, Baylor College of Medicine, Houston, Texas, USA.

Department of Molecular Virology and Microbiology, Baylor College of Medicine, Houston, Texas, USA.

出版信息

mBio. 2021 Apr 27;12(2):e00211-21. doi: 10.1128/mBio.00211-21.

Abstract

Extraintestinal pathogenic (ExPEC), often multidrug resistant (MDR), is a leading cause of urinary tract and systemic infections. The crisis of emergent MDR pathogens has led some to propose bacteriophages as a therapeutic. However, bacterial resistance to phage is a concerning issue that threatens to undermine phage therapy. Here, we demonstrate that sequence type 131, a circulating pandemic strain of ExPEC, rapidly develops resistance to a well-studied and therapeutically active phage (ϕHP3). Whole-genome sequencing of the resisters revealed truncations in genes involved in lipopolysaccharide (LPS) biosynthesis, the outer membrane transporter , or both, implicating them as phage receptors. We found ExPEC resistance to phage is associated with a loss of fitness in host microenvironments and attenuation in a murine model of systemic infection. Furthermore, we constructed a novel phage-bacterium bioreactor to generate an evolved phage isolate with restored infectivity to all LPS-truncated ExPEC resisters. This study suggests that although the resistance of pandemic to phage is frequent, it is associated with attenuation of virulence and susceptibility to new phage variants that arise by directed evolution. In response to the rising crisis of antimicrobial resistance, bacteriophage (phage) therapy has gained traction. In the United States, there have been over 10 cases of largely successful compassionate-use phage therapy to date. The resilience of pathogens allowing their broad antibiotic resistance means we must also consider resistance to therapeutic phages. This work fills gaps in knowledge regarding development of phage resisters in a model of infection and finds critical fitness losses in those resisters. We also found that the phage was able to rapidly readapt to these resisters.

摘要

肠外致病性(ExPEC),通常为多药耐药(MDR),是尿路感染和全身感染的主要原因。紧急出现的多药耐药病原体危机导致一些人提议使用噬菌体作为治疗方法。然而,细菌对噬菌体的耐药性是一个令人担忧的问题,有可能破坏噬菌体治疗。在这里,我们证明了血清型 131,一种循环的流行的 ExPEC 菌株,迅速对一种经过充分研究和具有治疗活性的噬菌体(ϕHP3)产生耐药性。耐药株的全基因组测序显示,参与脂多糖(LPS)生物合成、外膜转运体或两者的基因发生截断,暗示它们是噬菌体的受体。我们发现 ExPEC 对噬菌体的耐药性与在宿主微环境中丧失适应性和在全身感染的小鼠模型中减弱有关。此外,我们构建了一种新型噬菌体-细菌生物反应器,以产生一种具有恢复感染性的进化噬菌体分离株,可感染所有 LPS 截断的 ExPEC 耐药株。这项研究表明,尽管流行的血清型 131 对噬菌体的耐药性很常见,但它与毒力减弱有关,并且容易受到通过定向进化产生的新噬菌体变体的影响。为了应对抗菌药物耐药性不断上升的危机,噬菌体(噬菌体)治疗已经引起了关注。迄今为止,美国已经有超过 10 例基本上成功的同情用噬菌体治疗案例。病原体的弹性允许它们广泛的抗生素耐药性,这意味着我们还必须考虑对治疗性噬菌体的耐药性。这项工作填补了在感染模型中噬菌体耐药株发展的知识空白,并发现了这些耐药株的关键适应性丧失。我们还发现噬菌体能够迅速适应这些耐药株。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2d6f/8092219/4158892b1a6b/mBio.00211-21-f001.jpg

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