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噬菌体抗性进化诱导铜绿假单胞菌 PAO1 对特定抗生素的敏感性。

Phage Resistance Evolution Induces the Sensitivity of Specific Antibiotics in Pseudomonas aeruginosa PAO1.

机构信息

Food Safety Laboratory, College of Food Science and Engineering, Ocean University of Chinagrid.4422.0, Qingdao, China.

出版信息

Microbiol Spectr. 2022 Oct 26;10(5):e0135622. doi: 10.1128/spectrum.01356-22. Epub 2022 Aug 16.

Abstract

Bacteria frequently encounter selection by both phages and antibiotics. However, our knowledge on the evolutionary interactions between phages and antibiotics are still limited. Here, we characterized a phage-resistant Pseudomonas aeruginosa variant PAO1-R1 that shows increased sensitivity to gentamicin and polymyxin B. Using whole genome sequencing, significant genome differences were observed between the reference P. aeruginosa PAO1 and PAO1-R1. Compared to PAO1, 64 gene-encoding proteins with nonsynonymous single nucleotide polymorphisms (SNPs) and 31 genes with insertion/deletion (indel) mutations were found in PAO1-R1. We observed a significant reduction in phage adsorption rate for both phage vB_Pae_QDWS and vB_Pae_W3 against PAO1-R1 and proposed that disruption of phage adsorption is likely the main cause for evolving resistance. Because the majority of spontaneous mutations are closely related to membrane components, alterations in the cell envelope may explain the antibiotic-sensitive phenotype of PAO1-R1. Collectively, we demonstrate that the evolution of phage resistance comes with fitness defects resulting in antibiotic sensitization. Our finding provides new insights into the evolutionary interactions between resistance to the phage and sensitivity to antibiotics, which may have implications for the future clinical use of steering in phage therapies. Bacteria frequently encounter the selection pressure from both antibiotics and lytic phages. Little is known about the evolutionary interactions between antibiotics and phages. Our study provides new insights into the trade-off mechanism between resistance to the phage and sensitivity to antibiotics. This evolutionary trade-off is not dependent on the outer membrane proteins (OMPs) of the multidrug efflux pumps. The disruption of phage adsorption that induced phage resistance and the changes in structure or composition of membranes are presumably one of the major causes for antibiotic sensitivity. Our finding may fill some gaps in the field of phage-host interplay and have implications for the future clinical use of steering in phage therapies.

摘要

细菌经常同时面临噬菌体和抗生素的选择压力。然而,我们对噬菌体和抗生素之间的进化相互作用的了解仍然有限。在这里,我们描述了一种对噬菌体具有抗性的铜绿假单胞菌变体 PAO1-R1,该变体对庆大霉素和多粘菌素 B 的敏感性增加。通过全基因组测序,我们观察到参考铜绿假单胞菌 PAO1 和 PAO1-R1 之间存在显著的基因组差异。与 PAO1 相比,PAO1-R1 中有 64 个编码蛋白质的基因发生了非同义单核苷酸多态性(SNP),31 个基因发生了插入/缺失(indel)突变。我们观察到噬菌体 vB_Pae_QDWS 和 vB_Pae_W3 对 PAO1-R1 的吸附率显著降低,并提出噬菌体吸附的破坏可能是产生抗性的主要原因。由于大多数自发突变与膜成分密切相关,因此细胞包膜的改变可能解释了 PAO1-R1 对抗生素敏感的表型。总之,我们证明了噬菌体抗性的进化伴随着适应度缺陷,导致抗生素敏感性增加。我们的发现为噬菌体抗性和抗生素敏感性之间的进化相互作用提供了新的见解,这可能对未来噬菌体治疗中靶向的临床应用具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/10c6/9603957/b410451eaec7/spectrum.01356-22-f001.jpg

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