Please use this identifier to cite or link to this item: http://hdl.handle.net/1893/27786
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dc.contributor.authorMalik, Danish Jen_UK
dc.contributor.authorSokolov, Ilya Jen_UK
dc.contributor.authorVinner, Gurinder Ken_UK
dc.contributor.authorMancuso, Francescoen_UK
dc.contributor.authorCinquerrui, Salvatoreen_UK
dc.contributor.authorVladisavljevic, Goran Ten_UK
dc.contributor.authorClokie, Martha R Jen_UK
dc.contributor.authorGarton, Natalie Jen_UK
dc.contributor.authorStapley, Andrew G Fen_UK
dc.contributor.authorKirpichnikova, Annaen_UK
dc.date.accessioned2018-09-11T14:33:57Z-
dc.date.available2018-09-11T14:33:57Z-
dc.date.issued2017-11-30en_UK
dc.identifier.urihttp://hdl.handle.net/1893/27786-
dc.description.abstractAgainst a backdrop of global antibiotic resistance and increasing awareness of the importance of the human microbiota, there has been resurgent interest in the potential use of bacteriophages for therapeutic purposes, known as phage therapy. A number of phage therapy phase I and II clinical trials have concluded, and shown phages don't present significant adverse safety concerns. These clinical trials used simple phage suspensions without any formulation and phage stability was of secondary concern. Phages have a limited stability in solution, and undergo a significant drop in phage titre during processing and storage which is unacceptable if phages are to become regulated pharmaceuticals, where stable dosage and well defined pharmacokinetics and pharmacodynamics are de rigueur. Animal studies have shown that the efficacy of phage therapy outcomes depend on the phage concentration (i.e. the dose) delivered at the site of infection, and their ability to target and kill bacteria, arresting bacterial growth and clearing the infection. In addition, in vitro and animal studies have shown the importance of using phage cocktails rather than single phage preparations to achieve better therapy outcomes. The in vivo reduction of phage concentration due to interactions with host antibodies or other clearance mechanisms may necessitate repeated dosing of phages, or sustained release approaches. Modelling of phage-bacterium population dynamics reinforces these points. Surprisingly little attention has been devoted to the effect of formulation on phage therapy outcomes, given the need for phage cocktails, where each phage within a cocktail may require significantly different formulation to retain a high enough infective dose.en_UK
dc.language.isoenen_UK
dc.publisherElsevier BVen_UK
dc.relationMalik DJ, Sokolov IJ, Vinner GK, Mancuso F, Cinquerrui S, Vladisavljevic GT, Clokie MRJ, Garton NJ, Stapley AGF & Kirpichnikova A (2017) Formulation, stabilisation and encapsulation of bacteriophage for phage therapy. Advances in Colloid and Interface Science, 249, pp. 100-133. https://doi.org/10.1016/j.cis.2017.05.014en_UK
dc.rights© 2017 The Authors. Published by Elsevier B.V. This is an open access article under the CC BY license (http://creativecommons.org/licenses/BY/4.0/).en_UK
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/en_UK
dc.subjectPhysical and Theoretical Chemistryen_UK
dc.subjectColloid and Surface Chemistryen_UK
dc.subjectSurfaces and Interfacesen_UK
dc.titleFormulation, stabilisation and encapsulation of bacteriophage for phage therapyen_UK
dc.typeJournal Articleen_UK
dc.identifier.doi10.1016/j.cis.2017.05.014en_UK
dc.citation.jtitleAdvances in colloid and interface scienceen_UK
dc.citation.issn0001-8686en_UK
dc.citation.volume249en_UK
dc.citation.spage100en_UK
dc.citation.epage133en_UK
dc.citation.publicationstatusPublisheden_UK
dc.citation.peerreviewedRefereeden_UK
dc.type.statusVoR - Version of Recorden_UK
dc.contributor.funderEngineering and Physical Sciences Research Councilen_UK
dc.citation.date14/05/2017en_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationUniversity of Leicesteren_UK
dc.contributor.affiliationUniversity of Leicesteren_UK
dc.contributor.affiliationLoughborough Universityen_UK
dc.contributor.affiliationLiverpool Hope Universityen_UK
dc.identifier.wtid992322en_UK
dc.contributor.orcid0000-0001-5153-7375en_UK
dc.date.accepted2017-05-11en_UK
dcterms.dateAccepted2017-05-11en_UK
dc.date.filedepositdate2018-09-11en_UK
dc.subject.tagAgent-Based Simulationen_UK
dc.subject.tagInfectious Disease and Mathematical Modelsen_UK
dc.subject.tagMathematical Analysisen_UK
rioxxterms.apcnot requireden_UK
rioxxterms.typeJournal Article/Reviewen_UK
rioxxterms.versionVoRen_UK
local.rioxx.authorMalik, Danish J|en_UK
local.rioxx.authorSokolov, Ilya J|en_UK
local.rioxx.authorVinner, Gurinder K|en_UK
local.rioxx.authorMancuso, Francesco|en_UK
local.rioxx.authorCinquerrui, Salvatore|en_UK
local.rioxx.authorVladisavljevic, Goran T|en_UK
local.rioxx.authorClokie, Martha R J|en_UK
local.rioxx.authorGarton, Natalie J|en_UK
local.rioxx.authorStapley, Andrew G F|en_UK
local.rioxx.authorKirpichnikova, Anna|0000-0001-5153-7375en_UK
local.rioxx.projectEP/M027341/1|Engineering and Physical Sciences Research Council|http://dx.doi.org/10.13039/501100000266en_UK
local.rioxx.freetoreaddate2018-09-11en_UK
local.rioxx.licencehttp://creativecommons.org/licenses/by/4.0/|2018-09-11|en_UK
local.rioxx.filename1-s2.0-S000186861630392X-main.pdfen_UK
local.rioxx.filecount1en_UK
local.rioxx.source0001-8686en_UK
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