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Low-density neutrophil heterogeneity and spleen tyrosine kinase as therapeutic targets in sepsis
Heather L. Teague, Lauren Knabe, Raquel S. Da Cruz, Xianglan Yao, Kiana C. Allen, Trenton Williams, Cumhur Y. Demirkale, Merte Woldehanna, Ernest Evans, Amir Hobson, Jared D. Wilkinson, Steven D. Nathan, Christopher S. King, Jeffrey R. Strich
Heather L. Teague, Lauren Knabe, Raquel S. Da Cruz, Xianglan Yao, Kiana C. Allen, Trenton Williams, Cumhur Y. Demirkale, Merte Woldehanna, Ernest Evans, Amir Hobson, Jared D. Wilkinson, Steven D. Nathan, Christopher S. King, Jeffrey R. Strich
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Research Article Immunology Inflammation

Low-density neutrophil heterogeneity and spleen tyrosine kinase as therapeutic targets in sepsis

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Abstract

Sepsis is a leading cause of death for which host-directed therapies are urgently needed. We performed high-dimensional flow cytometry, measurement of soluble biomarkers, and lipopolysaccharide (LPS) stimulation of neutrophils to characterize neutrophil heterogeneity and function in patients with sepsis. We observed that in patients with sepsis, low-density neutrophils (LDNs) are elevated and phenotypically diverse populations of innate immune cells with varying degrees of maturity and myeloperoxidase expression. Spleen tyrosine kinase (SYK) expression was found to be higher in whole blood neutrophils and LDNs of patients with sepsis compared with healthy donors. Importantly, SYK+ LDNs associated with increased levels of intracellular myeloperoxidase (MPO) and soluble biomarkers. Furthermore, SYK+ LDNs correlated with clinical outcomes of sepsis disease severity, including sequential organ failure assessment score, mechanical ventilation, and vasopressors. Functionally, the SYK inhibitor R406 suppressed changes in neutrophil features of activation from normal-density neutrophils and LDNs, including the SYK+ and SYK– neutrophil subsets, and MPO release from LDNs following LPS stimulation of sepsis neutrophils. Combined, these results establish LDNs as a heterogenous population of neutrophils that express high levels of SYK and support SYK inhibition as a potentially novel therapeutic target aimed at suppressing overactive neutrophils in sepsis.

Authors

Heather L. Teague, Lauren Knabe, Raquel S. Da Cruz, Xianglan Yao, Kiana C. Allen, Trenton Williams, Cumhur Y. Demirkale, Merte Woldehanna, Ernest Evans, Amir Hobson, Jared D. Wilkinson, Steven D. Nathan, Christopher S. King, Jeffrey R. Strich

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Figure 4

Characterization of LDNs.

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Characterization of LDNs.
(A) optSNE plot of flow cytometry data overlai...
(A) optSNE plot of flow cytometry data overlaid with FlowSOM MCs for sepsis LDNs. (B) Abundance plot demonstrating the percentage of each MC. (C) Heatmap representing the relative expression of each extracellular and intracellular feature between MCs. (D) Histograms representing the relative expression of MPO across each MC. (E) optSNE plot of flow cytometry data overlaid with FlowSOM split by LDN-MC01 and LDN-MC02 combined and LDN-MC03 and LDN-MC04 combined. (F) Abundance plot demonstrating the percentage of MC01 and MC02 combined compared with MC03 and MC04 combined. (G) optSNE and bar graphs representing the expression of features in LDN-MC01 and LDN-MC02 compared with LDN-MC03 and LDN-MC04. (H) Correlation of LDN-MC01 and LDN-MC02 summed and LDN-MC03 and LDN-MC04 summed with SOFA score. Data are represented as means ± SEM. Significance was determined using a Friedman test, a paired t test, or a Wilcoxon test and set at P < 0.01**, P < 0.001***, P < 0.0001****. optSNE, optimized t-distributed stochastic neighbor embedding; MC, metacluster; MPO, myeloperoxidase; SEM, standard error of the mean.

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ISSN 2379-3708

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