Phage Therapy: The Pharmacology of Antibacterial Viruses

Danis-Wlodarczyk, Katarzyna; Dąbrowska, Krystyna; Abedon, Stephen T.

doi:10.21775/9781913652517.02

Cited by 6 publications

(8 citation statements)

References 185 publications

(224 reference statements)

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“…The role of bacteriophages as alternative antimicrobial agents has gained renewed interest in the past years ( 1 ). Enterohemorrhagic Escherichia coli (EHEC) strains, particularly of the O157:H7 serotype, are serious foodborne zoonotic pathogens, and several phages which show effective lysis of these have previously been characterized ( 2 , 3 ).…”

Section: Announcementmentioning

confidence: 99%

Complete Genome Sequences of Novel Bovine T4, rv5-Like, and Dhillonviruses Effective against Escherichia coli O157

Sváb

Falgenhauer

Chakraborty

et al. 2021

Microbiol Resour Announc

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Section: Announcementmentioning

confidence: 99%

Complete Genome Sequences of Novel Bovine T4, rv5-Like, and Dhillonviruses Effective against Escherichia coli O157

Sváb

Falgenhauer

Chakraborty

et al. 2021

Microbiol Resour Announc

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“…As a consequence, there can be no means of knowing how long initial phage doses are retained, whether phage numbers decline over time, or instead whether phage numbers increase in the course of phage in situ propagation ( Figure 3 ). In clinical settings, declines in concentrations of antibacterials found in association with targeted bacteria would suggest a need for drug re-application, and in clinical practice phages often are delivered not as only a single dose per treatment [ 72 , 73 , 74 , 75 , 76 , 77 , 78 , 79 ]. Thus, measuring phage titers over time, minimally such as at time zero in combination with end-point determinations, can be relevant to translating phage treatments of biofilm from in vitro or in vivo experimentation to clinical settings, or otherwise toward better appreciation of the ecology of phage-biofilm interactions.…”

Section: Improving Phage-biofilm In Vitro Experimentationmentioning

confidence: 99%

“…Note that in either case, at least in terms of phage treatments of in vitro biofilms, we can avoid these complications by starting with relatively high phage numbers, e.g., 10 7 PFU/mL or ideally [ 75 ] even higher. That is, when phages are applied to biofilms in higher numbers, then there should be less concern about the buildup of phage numbers around biofilms by means other than due to dosing or due to phage propagation within biofilms.…”

Section: Improving Phage-biofilm In Vitro Experimentationmentioning

confidence: 99%

“…Even if conditions are well matched between in situ and in vitro conditions, there can still be differences in biofilm properties that are a function simply of the duration of biofilm growth prior to phage application [ 163 ]. Indeed, this can occur in situ as well, perhaps most notably with distinctions in the characteristics of acute vs. chronic bacterial infections, which can also be a challenge to distinguish in terms of in vivo infection models [ 30 , 75 ]. Above all, we caution against assumptions of equivalence between in vitro-grown biofilms and those grown in situ, as well as in situ vs. ex situ phage treatments, unless such equivalence has been rigorously demonstrated.…”

Section: Improving Phage-biofilm In Vitro Experimentationmentioning

confidence: 99%

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Improving Phage-Biofilm In Vitro Experimentation

Abedon

Danis-Wlodarczyk

Wozniak

et al. 2021

Viruses

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Bacteriophages or phages, the viruses of bacteria, are abundant components of most ecosystems, including those where bacteria predominantly occupy biofilm niches. Understanding the phage impact on bacterial biofilms therefore can be crucial toward understanding both phage and bacterial ecology. Here, we take a critical look at the study of bacteriophage interactions with bacterial biofilms as carried out in vitro, since these studies serve as bases of our ecological and therapeutic understanding of phage impacts on biofilms. We suggest that phage-biofilm in vitro experiments often may be improved in terms of both design and interpretation. Specific issues discussed include (a) not distinguishing control of new biofilm growth from removal of existing biofilm, (b) inadequate descriptions of phage titers, (c) artificially small overlying fluid volumes, (d) limited explorations of treatment dosing and duration, (e) only end-point rather than kinetic analyses, (f) importance of distinguishing phage enzymatic from phage bacteriolytic anti-biofilm activities, (g) limitations of biofilm biomass determinations, (h) free-phage interference with viable-count determinations, and (i) importance of experimental conditions. Toward bettering understanding of the ecology of bacteriophage-biofilm interactions, and of phage-mediated biofilm disruption, we discuss here these various issues as well as provide tips toward improving experiments and their reporting.

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“…Однак перешкодами активного типу може бути те, що бактерії, які наявні в природному середовищі можуть бути менш фізіологічно активними та не підтримувати ті розміри фагових вибухів, які є в лабораторних умовах [14,15]. Водночас зміни у фізіології бактерій або зміни в експресії бактеріальних генів у відповідь на вплив зовнішніх чинників можуть зменшувати кількість молекул рецепторів на поверхні бактеріальної клітини, необхідних для адсорбції фагів [16,17]. Крім того не всі бактеріальні штами здатні підтримувати великі розміри вибуху або швидку адсорбцію віріонів.…”

Section: мікробіологія епізоотологія та інфекційні хворобиunclassified

Determination of the drug Fagomast effectiveness with different titers of Phage SAvB14

Horiuk

2021

Nauk. vìsn. vet. med.

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Treatment of bacterial infections with bacteriophages is one of the alternative methods. However, the use of freely dispersed bacteriophages for treatment causes their inactivation under physiological conditions. Therefore, it is important to consider the concentration of bacteriophages in phage therapy. The aim of study – to determine the optimal titer of bacteriophage Phage SAvB14 in the drug Fagomast for the effective treatment of subclinical mastitis in cows caused by Stapholococcus aureus var. bovis. For research to determine the optimal therapeutic dose of the bacteriophage drug Fagomast in vitro, groups of animals were formed on the principle of analogues. Controls were animals treated with an antibiotic-based drug according to the instructions for use. Cows of the first experimental group were used samples of the drug with a titer of Phage SAvB14 10-7 BFU/ml, the second experimental group with a titer of 10-8 BFU/ml and the third group – 10-9 BFU/ml. It was found that all batches of Fagomast (81.8 - 92.8%) show good therapeutic efficacy, but the duration of treatment of animals was different. When using the drug Fagomast with a phage titer of 10-9 BFU/ml, it is shorter by 1 day than cows that were injected with a phage titer of 10-8 BFU/ml and 1.5 days compared with cows of the first group, which were injected with a phage titer of 10-7 BFU/ml. The results of the therapeutic efficacy of Fagomast with a bacteriophage titer of 10-8 and 10-9 BFU/ml in the drug are confirmed by the reaction with Mastidine, which after 48 hours was assessed as doubtful, and after 72 hours – as negative, as with antibiotic treatment. The content of S. aureus in the secretion of cows 12 hours after administration of the drug with a phage titer of 10-9 BFU/ml decreased 6 times (P ≤ 0.05), and after 48 hours 40 times (P ≤ 0.05), and after 60 hours of therapy did not stand out at all. The titer of bacteriophages remained at the level of 10-7 BFU/ml, and when the number of susceptible bacteria decreased to zero it decreased by 2 orders of magnitude. Thus, it can be said that maintaining a higher concentration of phage virions leads to better distribution of phages in the breast, and thus to improved binding of phages to host cells and their destruction. Key words: bacteriophages, Staphylococcus aureus, phagotherapy, bacteriophage drug, mastitis, cows.

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Phage Therapy: The Pharmacology of Antibacterial Viruses

Cited by 6 publications

References 185 publications

Complete Genome Sequences of Novel Bovine T4, rv5-Like, and Dhillonviruses Effective against Escherichia coli O157

Complete Genome Sequences of Novel Bovine T4, rv5-Like, and Dhillonviruses Effective against Escherichia coli O157

Improving Phage-Biofilm In Vitro Experimentation

Determination of the drug Fagomast effectiveness with different titers of Phage SAvB14

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