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RESEARCH ARTICLE
Contents Vol 40(1)

Bacteriophage therapy for severe infections

Carola Venturini A B D , Aleksandra Petrovic Fabjian A and Ruby CY Lin A B C
+ Author Affiliations
- Author Affiliations

A Centre for Infectious Diseases and Microbiology, The Westmead Institute for Medical Research, Level 4, 176 Hawkesbury Road, Westmead, NSW 2145, Australia

B Sydney Medical School, Faculty of Medicine and Health, The University of Sydney, NSW 2000, Australia

C School of Medical Sciences, University of New South Wales, NSW 2052, Australia

D Tel: +61 2 8627 3415, Fax: +61 2 8627 3099, Email: carola.venturini@sydney.edu.au

Microbiology Australia 40(1) 20-23 https://doi.org/10.1071/MA19005
Published: 18 February 2019

Abstract

The rise of multiple antibiotic resistance in clinically relevant bacteria has created a global crisis with increasing burden on healthcare systems. The need to optimise alternative therapies to antibiotics, particularly in high risk nosocomial settings, is therefore immediate. Bacteriophages are specialised lethal viruses of bacteria, and an underused clinical resource for the treatment of severe infections refractory to antibiotics. Both the gaps in knowledge of bacteriophage biology, particularly the details of host-pathogen dynamic interactions, and legislative hurdles related to the regulation of natural microorganisms for therapy have delayed progress in bacteriophage clinical applications. At the Westmead Institute for Medical Research (WIMR), in collaboration with Westmead Hospital (Western Sydney Local Health District, WSLHD) and the University of Sydney (USyd), we have been investigating rational design protocols for routine bacteriophage application in clinical practice and testing bacteriophage therapeutics on patients suffering from multidrug resistant (MDR) severe infections.


References

[1]  Kutter, E. and Sulakvelidze, A. (2005) Bacteriophage therapy in humans. In Bacteriophages: biology and applications (Kutter, E. and Sulakvelidze, A., eds). pp. 372–427. CRC Press.

[2]  Chan, B.K. et al. (2013) Phage cocktails and the future of phage therapy. Future Microbiol. 8, 769–783.
Phage cocktails and the future of phage therapy.Crossref | GoogleScholarGoogle Scholar | 23701332PubMed |

[3]  Fokine, A. and Rossmann, M.G. (2014) Molecular architecture of tailed double-stranded DNA phages. Bacteriophage 4, e28281.
Molecular architecture of tailed double-stranded DNA phages.Crossref | GoogleScholarGoogle Scholar | 24616838PubMed |

[4]  Nobrega, F.L. et al. (2018) Targeting mechanisms of tailed bacteriophages. Nat. Rev. Microbiol. 16, 760–773.
Targeting mechanisms of tailed bacteriophages.Crossref | GoogleScholarGoogle Scholar | 30104690PubMed |

[5]  Sulakvelidze, A. et al. (2001) Bacteriophage therapy. Antimicrob. Agents Chemother. 45, 649–659.
Bacteriophage therapy.Crossref | GoogleScholarGoogle Scholar | 11181338PubMed |

[6]  Summers, W.C. (2012) The strange history of phage therapy. Bacteriophage 2, 130–133.
The strange history of phage therapy.Crossref | GoogleScholarGoogle Scholar | 23050223PubMed |

[7]  Pirnay, J.-P. et al. (2012) Introducing yesterday’s phage therapy in today’s medicine. Future Virol. 7, 379–390.
Introducing yesterday’s phage therapy in today’s medicine.Crossref | GoogleScholarGoogle Scholar |

[8]  Lin, D.M. et al. (2017) Phage therapy: an alternative to antibiotics in the age of multi-drug resistance. World J. Gastrointest. Pharmacol. Ther. 8, 162–173.
Phage therapy: an alternative to antibiotics in the age of multi-drug resistance.Crossref | GoogleScholarGoogle Scholar | 28828194PubMed |

[9]  Kutter, E. and Sulakvelidze, A. eds (2005) Bacteriophages: biology and applications. CRC Press.

[10]  Furfaro, L.L. et al. (2018) Bacteriophage therapy: clinical trials and regulatory hurdles. Front. Cell. Infect. Microbiol. 8, 376–382.
Bacteriophage therapy: clinical trials and regulatory hurdles.Crossref | GoogleScholarGoogle Scholar | 30406049PubMed |

[11]  Henein, A. (2013) What are the limitations on the wider therapeutic use of phage? Bacteriophage 3, e24872.
What are the limitations on the wider therapeutic use of phage?Crossref | GoogleScholarGoogle Scholar | 24228220PubMed |

[12]  Abedon, S.T. et al. (2017) Editorial: phage therapy: past, present and future. Front. Microbiol. 8, 981–987.
Editorial: phage therapy: past, present and future.Crossref | GoogleScholarGoogle Scholar | 28663740PubMed |

[13]  World Medical Association (2013) World medical association declaration of Helsinki: ethical principles for medical research involving human subjects. JAMA 310, 2191–2194.
World medical association declaration of Helsinki: ethical principles for medical research involving human subjects.Crossref | GoogleScholarGoogle Scholar | 24141714PubMed |

[14]  Debarbieux, L. et al. (2016) A bacteriophage journey at the European Medicines Agency. FEMS Microbiol. Lett. 363, fnv225.
A bacteriophage journey at the European Medicines Agency.Crossref | GoogleScholarGoogle Scholar | 26656541PubMed |

[15]  Maciejewska, B. et al. (2018) Applications of bacteriophages versus phage enzymes to combat and cure bacterial infections: an ambitious and also a realistic application? Appl. Microbiol. Biotechnol. 102, 2563–2581.
Applications of bacteriophages versus phage enzymes to combat and cure bacterial infections: an ambitious and also a realistic application?Crossref | GoogleScholarGoogle Scholar | 29442169PubMed |

[16]  Pirnay, J.P. et al. (2018) The magistral phage. Viruses 10, 64.
The magistral phage.Crossref | GoogleScholarGoogle Scholar |

[17]  Jault, P. et al. (2019) Efficacy and tolerability of a cocktail of bacteriophages to treat burn wounds infected by Pseudomonas aeruginosa (PhagoBurn): a randomised, controlled, double-blind phase 1/2 trial. Lancet Infect. Dis. 19, 35–45.
Efficacy and tolerability of a cocktail of bacteriophages to treat burn wounds infected by Pseudomonas aeruginosa (PhagoBurn): a randomised, controlled, double-blind phase 1/2 trial.Crossref | GoogleScholarGoogle Scholar | 30292481PubMed |

[18]  Abedon, S.T. Phage companies. http://www.companies.phage.org/ (accessed 28 December 2018).

[19]  Khawaldeh, A. et al. (2011) Bacteriophage therapy for refractory Pseudomonas aeruginosa urinary tract infection. J. Med. Microbiol. 60, 1697–1700.
Bacteriophage therapy for refractory Pseudomonas aeruginosa urinary tract infection.Crossref | GoogleScholarGoogle Scholar | 21737541PubMed |

[20]  Drilling, A.J. et al. (2017) Long-term safety of topical bacteriophage application to the frontal sinus region. Front. Cell. Infect. Microbiol. 7, 49–56.
Long-term safety of topical bacteriophage application to the frontal sinus region.Crossref | GoogleScholarGoogle Scholar | 28286740PubMed |

[21]  Aslam, S. et al. (2018) 1642. Safety and efficacy of bacteriophage therapy: analysis of clinical case series data. Open Forum Infect. Dis. 5, S47.
1642. Safety and efficacy of bacteriophage therapy: analysis of clinical case series data.Crossref | GoogleScholarGoogle Scholar |

[22]  Speck, P.G. and Wormald, P.J. ( ) Is phage therapy suitable for treating chronic sinusitis Staphylococcus aureus infection? Future Microbiol. 13, 605–608.
Is phage therapy suitable for treating chronic sinusitis Staphylococcus aureus infection?Crossref | GoogleScholarGoogle Scholar |