Neutrophil AKT2 regulates heterotypic cell-cell interactions during vascular inflammation
Jing Li, … , Xiaoping Du, Jaehyung Cho
Jing Li, … , Xiaoping Du, Jaehyung Cho
Published March 18, 2014
Citation Information: J Clin Invest. 2014;124(4):1483-1496. https://doi.org/10.1172/JCI72305.
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Research Article

Neutrophil AKT2 regulates heterotypic cell-cell interactions during vascular inflammation

Abstract

Interactions between platelets, leukocytes, and activated endothelial cells are important during microvascular occlusion; however, the regulatory mechanisms of these heterotypic cell-cell interactions remain unclear. Here, using intravital microscopy to evaluate mice lacking specific isoforms of the serine/threonine kinase AKT and bone marrow chimeras, we found that hematopoietic cell–associated AKT2 is important for neutrophil adhesion and crawling and neutrophil-platelet interactions on activated endothelial cells during TNF-α–induced venular inflammation. Studies with an AKT2-specific inhibitor and cells isolated from WT and Akt KO mice revealed that platelet- and neutrophil-associated AKT2 regulates heterotypic neutrophil-platelet aggregation under shear conditions. In particular, neutrophil AKT2 was critical for membrane translocation of αMβ2 integrin, β2-talin1 interaction, and intracellular Ca2+ mobilization. We found that the basal phosphorylation levels of AKT isoforms were markedly increased in neutrophils and platelets isolated from patients with sickle cell disease (SCD), an inherited hematological disorder associated with vascular inflammation and occlusion. AKT2 inhibition reduced heterotypic aggregation of neutrophils and platelets isolated from SCD patients and diminished neutrophil adhesion and neutrophil-platelet aggregation in SCD mice, thereby improving blood flow rates. Our results provide evidence that neutrophil AKT2 regulates αMβ2 integrin function and suggest that AKT2 is important for neutrophil recruitment and neutrophil-platelet interactions under thromboinflammatory conditions such as SCD.

Authors

Jing Li, Kyungho Kim, Eunsil Hahm, Robert Molokie, Nissim Hay, Victor R. Gordeuk, Xiaoping Du, Jaehyung Cho

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Figure 2

Hematopoietic cell AKT2 is important for neutrophil recruitment and neutrophil-platelet interactions on the TNF-α–inflamed endothelium.

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Hematopoietic cell AKT2 is important for neutrophil recruitment and neut...
Chimeric mice were generated by bone marrow transplantations in WT and Akt2 KO mice and used for intravital microscopy as described in Figure 1. (A) Number of adherent neutrophils. (B) Ratio of crawling/adherent neutrophils (percentage). (C) Median integrated fluorescence intensities of anti-CD42c antibodies (F platelets) were measured. Data represent the mean ± SEM (n = 60–64 venules in 8 mice per group). **P < 0.01 versus WT control mice by ANOVA and Dunnett’s test.