4.7 Article

Treatment with a neutrophil elastase inhibitor and ofloxacin reduces P. aeruginosa burden in a mouse model of chronic suppurative otitis media

Journal

NPJ BIOFILMS AND MICROBIOMES
Volume 7, Issue 1, Pages -

Publisher

NATURE RESEARCH
DOI: 10.1038/s41522-021-00200-z

Keywords

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Funding

  1. Department of Otolaryngology
  2. Stanford Initiative to Cure Hearing Loss
  3. NIH LRP from NCATS
  4. Stanford MCHRI through SPARK
  5. Stanford Bio-X USRP
  6. Action on Hearing Loss
  7. National Science Foundation [ECCS-1542152]
  8. SNSF Mini Seed Grant [S10RR027431-01]
  9. NIH [S10RR027431-01]

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This study identified Ly6G as the most informative factor driving disease in the CSOM mouse model, highlighting the role of neutrophils in the immune response. Neutrophil-specific immunomodulatory treatment significantly reduced bacterial burden in this model. Elevated levels of dsDNA in middle ear effusion samples may serve as a molecular biomarker of treatment response.
Chronic suppurative otitis media (CSOM) is a widespread, debilitating problem with poorly understood immunology. Here, we assess the host response to middle ear infection over the course of a month post-infection in a mouse model of CSOM and in human subjects with the disease. Using multiparameter flow cytometry and a binomial generalized linear machine learning model, we identified Ly6G, a surface marker of mature neutrophils, as the most informative factor of host response driving disease in the CSOM mouse model. Consistent with this, neutrophils were the most abundant cell type in infected mice and Ly6G expression tracked with the course of infection. Moreover, neutrophil-specific immunomodulatory treatment using the neutrophil elastase inhibitor GW 311616A significantly reduces bacterial burden relative to ofloxacin-only treated animals in this model. The levels of dsDNA in middle ear effusion samples are elevated in both humans and mice with CSOM and decreased during treatment, suggesting that dsDNA may serve as a molecular biomarker of treatment response. Together these data strongly implicate neutrophils in the ineffective immune response to P. aeruginosa infection in CSOM and suggest that immunomodulatory strategies may benefit drug-tolerant infections for chronic biofilm-mediated disease.

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