Neutrophils from critically ill septic patients mediate profound loss of endothelial barrier integrity
TL;DR: Neutrophils from septic patients exert dramatic compromise of endothelial barrier integrity, which depends upon the initial inflammatory event, correlates with organ dysfunction and resolution of sepsis, and is ameliorated by β-glucan.
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Abstract: Sepsis is characterized by systemic immune activation and neutrophil-mediated endothelial barrier integrity compromise, contributing to end-organ dysfunction. Studies evaluating endothelial barrier dysfunction induced by neutrophils from septic patients are lacking, despite its clinical significance. We hypothesized that septic neutrophils would cause characteristic patterns of endothelial barrier dysfunction, distinct from experimental stimulation of normal neutrophils, and that treatment with the immunomodulatory drug β-glucan would attenuate this effect. Blood was obtained from critically ill septic patients. Patients were either general surgery patients (Primary Sepsis (PS)) or those with sepsis following trauma (Secondary Sepsis (SS)). Those with acute respiratory distress syndrome (ARDS) were identified. Healthy volunteers served as controls. Neutrophils were purified and aliquots were untreated, or treated with fMLP or β-glucan. Endothelial cells were grown to confluence and activated with tissue necrosis factor (TNF)-α . Electric Cell-substrate Impedance Sensing (ECIS) was used to determine monolayer resistance after neutrophils were added. Groups were analyzed by two-way analysis of variance (ANOVA). Neutrophils from all septic patients, as well as fMLP-normal neutrophils, reduced endothelial barrier integrity to a greater extent than untreated normal neutrophils (normalized resistance of cells from septic patients at 30 mins = 0.90 ± 0.04; at 60 mins = 0.73 ± 0.6 and at 180 mins = 0.56 ± 0.05; p < 0. 05 vs normal). Compared to untreated PS neutrophils, fMLP-treated PS neutrophils caused further loss of barrier function at all time points; no additive effect was noted in stimulation of SS neutrophils beyond 30 min. Neutrophils from ARDS patients caused greater loss of barrier integrity than those from non-ARDS patients, despite similarities in age, sex, septic source, and neutrophil count. Neutrophils obtained after resolution of sepsis caused less barrier dysfunction at all time points. β-glucan treatment of septic patients’ neutrophils attenuated barrier compromise, rendering the effect similar to that induced by neutrophils obtained once sepsis had resolved. Neutrophils from septic patients exert dramatic compromise of endothelial barrier integrity. This pattern is mimicked by experimental activation of healthy neutrophils. The effect of septic neutrophils on the endothelium depends upon the initial inflammatory event, correlates with organ dysfunction and resolution of sepsis, and is ameliorated by β-glucan.
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Single-cell RNA sequencing reveals multiple pathways involving pulmonary immune and epithelial cells through which aryl hydrocarbon receptor activation attenuates acute respiratory distress syndrome
Ahmed K Aladhami,Taylor H Carter,Shruthi Thada,Prakash S Nagarkatti,Mitzi Nagarkatti +4 more
Abstract: Abstract Acute respiratory distress syndrome (ARDS) is a severe inflammatory lung disorder triggered by pneumonia, sepsis, trauma, and COVID-19, leading to high mortality. In this study, we investigated the effect of aryl hydrocarbon receptor (AhR) activation by 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD), a potent ligand, on LPS-induced ARDS in mice using single-cell RNA sequencing (scRNA-seq). scRNA-seq revealed 16 transcriptionally distinct cell clusters in the lungs. AhR activation reversed the decreased pulmonary functions caused by LPS, and significantly reduced pulmonary infiltration of monocytes, neutrophils, and macrophages. Interestingly, AhR activation during ARDS led to increased proportions of alveolar macrophages and angiogenic and quiescent endothelial cells. Among the downregulated pathways, prostaglandin signaling was the most broadly suppressed across many cell types in the LPS + TCDD group. AhR activation suppressed the neutrophil chemotaxis pathway involving Cxcl2, Cxcl3, and Cxcl10. The damage to endothelial and epithelial cells induced during ARDS was also blocked by AhR activation. This was associated with decreased expression of S100a8 and S100a9. Notably, multiple pathways related to cellular junction organization were enriched following AhR activation. Additionally, Scgb1a1, also called club cell protein 16 (CC16), primarily secreted by club cells in the respiratory epithelium, was highly upregulated following AhR activation, accounting for lung homeostasis. Together, these findings demonstrate that AhR activation mitigates key inflammatory and barrier-disruptive processes involving multiple cell types in LPS-induced ARDS. These data identify AhR as a central regulator of pulmonary inflammation and epithelial–endothelial integrity and support the future evaluation of AhR-targeted therapeutics as potential treatment for ARDS.
Cannabis Sativa Revisited-Crosstalk between microRNA Expression, Inflammation, Oxidative Stress, and Endocannabinoid Response System in Critically Ill Patients with Sepsis.
Anca Dinu,Alexandru Florin Rogobete,Tiberiu Bratu,Sonia Elena Popovici,Ovidiu Horea Bedreag,Marius Papurica,Lavinia Melania Bratu,Dorel Sandesc +7 more
TL;DR: The aim of this review paper was to present, in detail, the important mechanisms modulated by the endocannabinoid signaling pathway, as well as of the molecular and cellular links it has with sepsis.
Mitochondrial activity promotes neutrophil degranulation and endothelial dysfunction in systemic infections
Przemysław Zakrzewski,Christopher M. Rice,Claire Naveh,Isaac Dowell,Kathryn Fleming,Aravind V Ramesh,Rachel Jones,Pedro L. Moura,Drinalda Cela,Sarah Groves,Stephanie Fletcher-Jones,Yohance Victory,Mainga Bhima,Stefan Ebmeier,Laura Carey,Matthew Butler,Simon C Satchell,Ase Berg,Nadia Palolite,James Nyirenda,Watipenge Nyasulu,Isabel Zgambo,Charalampos Attipa,Linda Wooldridge,Andrew Davidson,Aubrey Cunnington,Christopher A. Moxon,Borko Amulic,Przemysław Zakrzewski,Christopher M. Rice,Claire Naveh,Isaac Dowell,Kathryn Fleming,Aravind V Ramesh,Rachel Jones,Pedro L. Moura,Drinalda Cela,Sarah Groves,Stephanie Fletcher-Jones,Yohance Victory,Mainga Bhima,Stefan Ebmeier,Laura Carey,Matthew Butler,Simon C Satchell,Ase Berg,Nadia Palolite,James Nyirenda,Watipenge Nyasulu,Isabel Zgambo,Charalampos Attipa,Linda Wooldridge,Andrew Davidson,Aubrey Cunnington,Christopher A. Moxon,Borko Amulic,Przemysław Zakrzewski,Andrew D. Davidson,Aubrey J. Cunnington,Christopher A. Moxon +59 more
- 13 Oct 2025
Abstract: ABSTRACT Neutrophils are essential for defense against pathogens but excessive activation in systemic infections can drive immunopathology. We show that neutrophil degranulation can induce endothelial dysfunction via degradation of the glycocalyx and increase of endothelial permeability. To identify targetable pathways regulating neutrophil degranulation in severe inflammation, we compared the proteomes of neutrophils isolated from patients with severe malaria and sepsis. We found significant upregulation of mitochondrial pathways, which was accompanied by increased rates of mitochondrial respiration and was linked to neutrophil immaturity. Malaria induced mitochondrial fusion and networking, while sepsis was associated with mitochondrial biogenesis. Immature neutrophils in both infections produced elevated levels of mitochondrial ROS, which enhanced release of primary and secondary granules. Our study provides a mechanistic explanation for the hyperinflammatory nature of immature neutrophils and points to pharmacological scavenging of mitochondrial ROS as a potential therapeutic strategy to reduce endothelial damage in severe inflammation.
The association between neutrophil-to-lymphocyte count ratio and mortality in septic patients: a retrospective analysis of the MIMIC-III database
Weiyan Ye,Xiaoli Chen,Yongbo Huang,Yuchong Li,Yonghao Xu,Zhenting Liang,Danlin Wu,Xiaoqing Liu,Yimin Li +8 more
TL;DR: High NLCR (>20.25) is independently related to increased 28-day all-cause mortality in adult septic patients of a limited sensibility and specificity, and further large multi-center prospective studies are needed to confirm such relationship and to validate whose clinical significance.
Neutrophil Extracellular Traps Induced by Shiga Toxin and Lipopolysaccharide-Treated Platelets Exacerbate Endothelial Cell Damage
Verónica Inés Landoni,Jose R Pittaluga,Agostina Carestia,Luis A. Castillo,Marcelo de Campos Nebel,Daiana Martire-Greco,Federico Birnberg-Weiss,Mirta Schattner,Pablo Schierloh,Gabriela C. Fernández +9 more
TL;DR: Systemic endothelial damage/dysfunction was decreased when NETs were disrupted, or when Plts were depleted, indicating that the promotion of netosis by Plts in the context of LPS and Stx2 plays a fundamental role in endothelial toxicity.
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