Relevance of the bacteriophage adherence to mucus model for Pseudomonas aeruginosa phages

Author:

Almeida Gabriel Magno de Freitas1ORCID,Ravantti Janne2,Grdzelishvili Nino34,Kakabadze Elene3,Bakuradze Nata3,Javakhishvili Elene3,Megremis Spyridon5,Chanishvili Nina3,Papadopoulos Nikolaos5,Sundberg Lotta-Riina6ORCID

Affiliation:

1. Faculty of Biosciences, Fisheries and Economics, The Norwegian College of Fishery Science, UiT—The Arctic University of Norway, Tromsø, Norway

2. Molecular and Integrative Biosciences Research Programme, University of Helsinki, Helsinki, Finland

3. George Eliava Institute of Bacteriophages, Microbiology & Virology, Tbilisi, Georgia

4. Faculty of Natural Science and Medicine, Ilia State University, Tbilisi, Georgia

5. University of Manchester, Manchester, United Kingdom

6. Department of Biological and Environmental Science and Nanoscience Centre, University of Jyväskylä, Jyväskylä, Finland

Abstract

ABSTRACT Pseudomonas aeruginosa infections are getting increasingly serious as antimicrobial resistance spreads. Phage therapy may be a solution to the problem, especially if improved by current advances on phage-host studies. As a mucosal pathogen, we hypothesize that P. aeruginosa and its phages are linked to the bacteriophage adherence to mucus (BAM) model. This means that phage-host interactions could be influenced by mucin presence, impacting the success of phage infections on the P. aeruginosa host and consequently leading to the protection of the metazoan host. By using a group of four different phages, we tested three important phenotypes associated with the BAM model: phage binding to mucin, phage growth in mucin-exposed hosts, and the influence of mucin on CRISPR immunity of the bacterium. Three of the tested phages significantly bound to mucin, while two had improved growth rates in mucin-exposed hosts. Improved phage growth was likely the result of phage exploitation of mucin-induced physiological changes in the host. We could not detect CRISPR activity in our system but identified two putative anti-CRISPR proteins coded by the phage. Overall, the differential responses seen for the phages tested show that the same bacterial species can be targeted by mucosal-associated phages or by phages not affected by mucus presence. In conclusion, the BAM model is relevant for phage-bacterium interactions in P. aeruginosa , opening new possibilities to improve phage therapy against this important pathogen by considering mucosal interaction dynamics. IMPORTANCE Some bacteriophages are involved in a symbiotic relationship with animals, in which phages held in mucosal surfaces protect them from invading bacteria. Pseudomonas aeruginosa is one of the many bacterial pathogens threatening humankind during the current antimicrobial resistance crisis. Here, we have tested whether P. aeruginosa and its phages are affected by mucosal conditions. We discovered by using a collection of four phages that, indeed, mucosal interaction dynamics can be seen in this model. Three of the tested phages significantly bound to mucin, while two had improved growth rates in mucin-exposed hosts. These results link P. aeruginosa and its phages to the bacteriophage adherence to the mucus model and open opportunities to explore this to improve phage therapy, be it by exploiting the phenotypes detected or by actively selecting mucosal-adapted phages for treatment.

Funder

Research Council of Finland

EC | Horizon 2020 Framework Programme

Publisher

American Society for Microbiology

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