4.7 Article

Bacteriophage uptake by mammalian cell layers represents a potential sink that may impact phage therapy

期刊

ISCIENCE
卷 24, 期 4, 页码 -

出版社

CELL PRESS
DOI: 10.1016/j.isci.2021.102287

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资金

  1. Monash Graduate Scholarship (MGS)
  2. Australia-Americas PhD Research Internship Program through the Australian Academy of Science
  3. CSIRO's Probing Biosystems Future Science Platform
  4. ARC Training Center for Personalised Therapeutic Technologies [IC170100016]
  5. Australian Research Council DECRA Fellowship [DE170100525]
  6. National Health and Medical Research Council [NHMRC: 1156588]
  7. Perpetual Trustees Australia award [2018HIG00007]
  8. Australian Research Council [IC170100016, DE170100525] Funding Source: Australian Research Council

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It has been found that bacteriophages have tropisms beyond their bacterial hosts and can adhere to mammalian tissues before being internalized through processes like macropinocytosis. Understanding these interactions may have significant implications on immune responses, phage pharmacokinetics, and the efficacy of phage therapy.
It is increasingly apparent that bacteriophages, viruses that infect bacteria and more commonly referred to as simply phages, have tropisms outside their bacterial hosts. Using live tissue culture cell imaging, we demonstrate that cell type, phage size, and morphology play a major role in phage internalization. Uptake was validated under physiological conditions using a microfluidic device. Phages adhered to mammalian tissues, with adherent phages being subsequently internalized by macropinocytosis, with functional phages accumulating intracellularly. We incorporated these results into a pharmacokinetic model demonstrating the potential impact of phage accumulation by cell layers, which represents a potential sink for circulating phages in the body. During phage therapy, high doses of phages are directly administered to a patient in order to treat a bacterial infection, thereby facilitating broad interactions between phages and mammalian cells. Understanding these interactions will have important implications on innate immune responses, phage pharmacokinetics, and the efficacy of phage therapy.

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