Csk-mediated Src family kinase regulation dampens neutrophil infiltration during pulmonary infection
Wida Amini, Lena Schemmelmann, Jan-Niklas Heming, Marina Oguama, Katharina Thomas, Helena Block, Pia Lindental, Bernadette Bardel, Andreas Margraf, Oliver Soehnlein, Anika Cappenberg, Alexander Zarbock
Wida Amini, Lena Schemmelmann, Jan-Niklas Heming, Marina Oguama, Katharina Thomas, Helena Block, Pia Lindental, Bernadette Bardel, Andreas Margraf, Oliver Soehnlein, Anika Cappenberg, Alexander Zarbock
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Research Article Immunology Inflammation

Csk-mediated Src family kinase regulation dampens neutrophil infiltration during pulmonary infection

Abstract

Neutrophil recruitment is crucial for pathogen elimination. However, precise control of the inflammatory response prevents overshooting reactions. Neutrophil activation initiates signaling, resulting in integrin β2 (Itgb2) activation and neutrophil arrest. Src family kinases are involved in multiple cellular processes and are negatively regulated by the C-terminal Src kinase (Csk). During this study, we investigated the mechanism by which Csk regulates integrin activation and neutrophil recruitment. Here, we demonstrated that Csk deficiency in murine neutrophils resulted in increased neutrophil adhesion to the endothelium along with decreased neutrophil transmigration into inflamed tissues compared with their littermate controls. In bacterial pneumonia, infected Csk-deficient mice showed higher bacterial burdens and decreased neutrophil recruitment, while other immune cell counts and cytokine levels were not significantly different compared to control. Analyses of Csk-deficient neutrophils revealed an increased Itgb2 affinity, leading to reduced migration and intravascular crawling. Mechanistically, elevated cAMP levels increased protein kinase A activity, which subsequently enhanced Csk activation. Csk, in turn, suppressed Src family kinase activation through phosphorylation (Y529). Hence, Csk-mediated regulation of neutrophil infiltration contributes to maintain a balanced immune response during bacterial pneumonia.

Authors

Wida Amini, Lena Schemmelmann, Jan-Niklas Heming, Marina Oguama, Katharina Thomas, Helena Block, Pia Lindental, Bernadette Bardel, Andreas Margraf, Oliver Soehnlein, Anika Cappenberg, Alexander Zarbock

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Figure 1

Csk is crucial for neutrophil recruitment and bacterial clearance in K. pneumoniae–induced pneumonia.

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Csk is crucial for neutrophil recruitment and bacterial clearance in K. ...
(AK) Cskfl/flLyz2wt/wt and Cskfl/flLyz2cre/wt mice were subjected to K. pneumoniae intratracheal injection or sham surgery. After 24 hours, bacterial burden regarding the colony forming units (CFUs) in lung (A), bronchoalveolar fluid (BALF) (B), blood (C), and spleen (D) and neutrophil recruitment into the lungs (E) and BALF (F) were determined. (G) Neutrophil recruitment (CD45+Gr-1+LyB.2+) in Cskfl/flLyz2wt/wt and Cskfl/flLyz2cre/wt mice in the interstitial, intravascular, and BALF compartments following intratracheal instillation of K. pneumoniae. Cell count of monocytes (MO; CD45+CD11b+CX3CR1+Ly6ChiLy6GGr-1) (H), alveolar macrophages (AM; CD45+CD64+F4/80+MARCO+SiglecFhi) (I), natural killer cells (NK; CD45+CD27+CD335+) (J), and dendritic cells (DC; CD45+CD27CD24+CD11c+MHCII+) (K) in lung tissue 24 hours after lung infection. n as indicated, mean ± SEM. *P < 0.05; **P < 0.01; ***P < 0.001; ****P < 0.0001 by 1-way-ANOVA by Holm-Šídák multiple-comparison test (AD), 1-way ANOVA with Tukey’s multiple-comparison test (E, F, and HK), or 2-tailed Student’s t test (G).