Post-Endotoxin Exposure-Induced Lung Inflammation and Resolution Consequences Beneficially Impacted by Lung-Delivered IL-10 Therapy

Authors

Jill A. Poole, University of Nebraska Medical CenterFollow
Rohit Gaurav, University of Nebraska Medical CenterFollow
Aaron Schwab, University of Nebraska Medical CenterFollow
Amy J. Nelson, University of Nebraska Medical CenterFollow
Angela Gleason, University of Nebraska Medical CenterFollow
Debra J. Romberger, University of Nebraska Medical CenterFollow
Todd A. Wyatt, University of Nebraska Medical CenterFollow

Document Type

Article

Journal Title

Scientific Reports

Publication Date

2022

Volume

12

Abstract

Although lung diseases typically result from long-term exposures, even a robust, one-time exposure can result in long-lasting consequences. Endotoxin is a ubiquitous environmental/occupational inflammatory agent often used to model airway inflammation. Using a murine model, the return to lung homeostasis following high dose inhalant lipopolysaccharide (LPS, 10-100 μg) exposure were delineated over 2 weeks. LPS-induced rapid weight loss, release of proinflammatory mediators, and inflammatory cell influx with prolonged persistence of activated macrophages CD11c⁺CD11b⁺ and recruited/transitioning CD11c^intCD11b⁺ monocyte-macrophages out to 2 weeks. Next, lung-delivered recombinant (r) interleukin (IL)-10 was intratracheally administered for 3 doses initiated 5 h following LPS (10 μg) exposure for 2 days. IL-10 therapy reduced LPS-induced weight loss and increased blood glucose levels. Whereas there was no difference in LPS-induced bronchoalveolar lavage airway fluid cellular influx, total lung cell infiltrates were reduced (37%) with rIL-10 treatment. Post-LPS exposure treatment with rIL-10 strikingly reduced lavage fluid and lung homogenate levels of tumor necrosis factor-α (88% and 93% reduction, respectively), IL-6 (98% and 94% reduction), CXCL1 (66% and 75% reduction), and CXCL2 (47% and 67% reduction). LPS-induced recruited monocyte-macrophages (CD11c^intCD11b⁺) were reduced (68%) with rIL-10. Correspondingly, LPS-induced lung tissue CCR2⁺ inflammatory monocyte-macrophage were reduced with rIL-10. There were also reductions in LPS-induced lung neutrophils, lymphocyte subpopulations, collagen content, and vimentin expression. These findings support the importance of studying resolution processes for the development of treatment after unintended environmental/occupational biohazard exposures. Short-term, lung-delivered rIL-10 favorably hastened inflammatory recovery processes following acute, high dose inhalant LPS exposure.

MeSH Headings

Animals, Blood Glucose, Bronchoalveolar Lavage Fluid, CD11c Antigen, Endotoxins, Hazardous Substances, Inflammation, Interleukin-10, Interleukin-6, Lipopolysaccharides, Lung, Mice, Pneumonia, Tumor Necrosis Factor-alpha, Vimentin, Weight Loss

DOI Link

10.1038/s41598-022-22346-2

ISSN

2045-2322

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Recommended Citation

Poole, Jill A.; Gaurav, Rohit; Schwab, Aaron; Nelson, Amy J.; Gleason, Angela; Romberger, Debra J.; and Wyatt, Todd A., "Post-Endotoxin Exposure-Induced Lung Inflammation and Resolution Consequences Beneficially Impacted by Lung-Delivered IL-10 Therapy" (2022). Journal Articles: Environmental, Agricultural & Occupational Health. 16.
https://digitalcommons.unmc.edu/coph_env_articles/16