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Emerging bacterial antibiotic resistance draws attention to bacteriophages as a therapeutic alternative to treat bacterial infection. Examples of phage that combat bacteria abound. However, despite careful testing of antibacterial activity in vitro, failures nevertheless commonly occur. We investigated immunological response of phage antibacterial potency in vivo. Anti-phage activity of phagocytes, antibodies, and serum complement were identified by direct testing and by high-resolution fluorescent microscopy. We accommodated the experimental data into a mathematical model. We propose a universal schema of innate and adaptive immunity impact on phage pharmacokinetics, based on the results of our numerical simulations. We found that the mammalian-host response to infecting bacteria causes the concomitant removal of phage from the system. We propose the notion that this effect as an indirect pathway of phage inhibition by bacteria with significant relevance for the clinical outcome of phage therapy.
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Hodyra‐Stefaniak et al. (Tue,) studied this question.
synapsesocial.com/papers/69de5c03a051b8e25be93d94 — DOI: https://doi.org/10.1038/srep14802
Katarzyna Hodyra‐Stefaniak
Silesian Center for Heart Disease
Paulina Miernikiewicz
Ludwik Hirszfeld Institute of Immunology and Experimental Therapy
Jarosław Drapała
Wrocław University of Science and Technology
Scientific Reports
Wrocław University of Science and Technology
Institute of Computer Science
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