Immunomodulation of neutrophil granulocyte functions by bacterial polyphosphates

Author:

Krenzlin Viola1,Schöche Johannes1,Walachowski Sarah2,Reinhardt Christoph1ORCID,Radsak Markus P.345ORCID,Bosmann Markus125ORCID

Affiliation:

1. Center for Thrombosis and Hemostasis University Medical Center of the Johannes Gutenberg‐University Mainz Mainz Germany

2. Pulmonary Center Department of Medicine Boston University School of Medicine Boston MA USA

3. Third Department of Medicine‐Hematology and Oncology University Medical Center of the Johannes Gutenberg‐University Mainz Mainz Germany

4. Mainz Research School of Translational Biomedicine (TransMed) University Medical Center of the Johannes Gutenberg‐University Mainz Mainz Germany

5. Research Center for Immunotherapy (FZI) University Medical Center of the Johannes Gutenberg‐University Mainz Mainz Germany

Abstract

AbstractPolyphosphates are highly conserved, linear polymers of monophosphates that reside in all living cells. Bacteria produce long chains containing hundreds to thousands of phosphate units, which can interfere with host defense to infection. Here, we report that intratracheal long‐chain polyphosphate administration to C57BL/6J mice resulted in the release of proinflammatory cytokines and influx of Ly6G+ polymorphonuclear neutrophils in the bronchoalveolar lavage fluid causing a disruption of the physiologic endothelial–epithelial small airway barrier and histologic signs of lung injury. Polyphosphate‐induced effects were attenuated after neutrophil depletion in mice. In isolated murine neutrophils, long‐chain polyphosphates modulated cytokine release induced by lipopolysaccharides (LPS) from Gram‐negative bacteria or lipoteichoic acid from Gram‐positive bacteria. In addition, long‐chain polyphosphates induced immune evasive effects in human neutrophils. In detail, long‐chain polyphosphates downregulated CD11b and curtailed the phagocytosis of Escherichia coli particles by neutrophils. Polyphosphates modulated the migration capacity by inducing CD62L shedding resulting in CD62Llow and CD11blow neutrophils. The release of IL‐8 induced by LPS was also significantly reduced. Pharmacologic blockade of PI3K with wortmannin antagonized long‐chain polyphosphate‐induced effects on LPS‐induced IL‐8 release.In conclusion, polyphosphates govern immunomodulation in murine and human neutrophils, suggesting polyphosphates as a therapeutic target for bacterial infections to restore innate immune defense.

Publisher

Wiley

Subject

Immunology,Immunology and Allergy

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