Survival during influenza-associated bacterial superinfection improves following viral- and bacterial-specific monoclonal antibody treatment
Keven M. Robinson, … , Taylor S. Cohen, John F. Alcorn
Keven M. Robinson, … , Taylor S. Cohen, John F. Alcorn
Published July 25, 2019
Citation Information: JCI Insight. 2019;4(14):e125554. https://doi.org/10.1172/jci.insight.125554.
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Research Article Immunology Infectious disease

Survival during influenza-associated bacterial superinfection improves following viral- and bacterial-specific monoclonal antibody treatment

Abstract

Postinfluenza bacterial superinfections cause increased morbidity and mortality compared with singular infection with influenza during both pandemics and seasonal epidemics. Vaccines and current treatments provide limited benefit, a rationale to conduct studies utilizing alternative therapies. FY1 and an optimized version, MEDI8852, anti-influenza HA mAbs, have been shown to neutralize influenza virus during singular influenza infection. MEDI4893*, an anti–Staphylococcus aureus α-toxin mAb, has been shown to improve survival when administered prophylactically prior to S. aureus pneumonia. Our objective was to determine if mAbs can improve survival during postinfluenza bacterial pneumonia. We administered FY1 in a murine model of postinfluenza methicillin-resistant S. aureus (MRSA) pneumonia and observed improved survival rates when given early during the course of influenza infection. Our findings indicate decreased lung injury and increased uptake and binding of bacteria by macrophages in the mice that received FY1 earlier in the course of influenza infection, corresponding to decreased bacterial burden. We also observed improved survival when mice were treated with a combination of FY1 and MEDI4893* late during the course of postinfluenza MRSA pneumonia. In conclusion, both FY1 and MEDI4893* prolong survival when used in a murine model of postinfluenza MRSA pneumonia, suggesting pathogen-specific mAbs as a possible therapeutic in the context of bacterial superinfection.

Authors

Keven M. Robinson, Krishnaveni Ramanan, Joshua M. Tobin, Kara L. Nickolich, Matthew J. Pilewski, Nicole L. Kallewaard, Bret R. Sellman, Taylor S. Cohen, John F. Alcorn

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Figure 5

Neutrophils are not required for protection from influenza HA targeting mAb, but influenza HA targeting mAb enhances macrophage uptake of bacteria.

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Neutrophils are not required for protection from influenza HA targeting ...
C57BL/6 mice infected with 100 PFUs of influenza A PR/8/34 received a single dose of FY1 on day 1 after influenza infection. Mice received neutrophil depletion antibody 1A8 (anti Ly6G) or IgG control at 48, 24, and 2 hours prior to secondary infection with 5 × 107 CFUs of MRSA on day 6 after influenza infection. Samples were harvested 24 hours following bacterial infection. (A) Bacterial colony counts in the lung (n = 6). C57BL/6 mice infected with 100 PFUs of influenza A PR/8/34 received a single dose of FY1 on day 1 after influenza infection. Mice received 5 x 107 CFUs of FITC-labeled MRSA on day 6 after influenza. Samples were harvested 24 hours following bacterial infection (n = 6). (B) Percentage of FITC+CD11b+Ly6G+ cells in lung by flow cytometry. (C) Percentage of FITC+F480+SiglecF+ cells in lung by flow cytometry. (D) Percentage of FITC+F480+SiglecF cells in lung by flow cytometry. Significance was tested by unpaired t test. Data represent mean ± SEM.