In ALI, inflammation from lipopolysaccharide (LPS) or other pathogens induces generation of unknown platelet GPVI activators. Although fibrin is a strong potential agonist, histones, collagen, or other agonists could be generated to activate GPVI. GPVI activation induces platelet-dependent neutrophil (PMN) recruitment and firm adhesion to the endothelium. This allows for neutrophils to migrate into the alveolar space. In addition, platelet-dependent neutrophil activation can lead to neutrophil extracellular trap formation (NETosis). Overall, the formation of platelet-neutrophil complexes (PNCs) leads to increased edema, brochoalevolar lavage (BAL) proteins, and cytokine generation. Inhibition of GPVI through either genetic deletion or anti-GPVI antibodies decreases neutrophil recruitment and activation, leading to reduced lung damage and hypoxia. Figure prepared with assistance from Diana Lim.

In ALI, inflammation from lipopolysaccharide (LPS) or other pathogens induces generation of unknown platelet GPVI activators. Although fibrin is a strong potential agonist, histones, collagen, or other agonists could be generated to activate GPVI. GPVI activation induces platelet-dependent neutrophil (PMN) recruitment and firm adhesion to the endothelium. This allows for neutrophils to migrate into the alveolar space. In addition, platelet-dependent neutrophil activation can lead to neutrophil extracellular trap formation (NETosis). Overall, the formation of platelet-neutrophil complexes (PNCs) leads to increased edema, brochoalevolar lavage (BAL) proteins, and cytokine generation. Inhibition of GPVI through either genetic deletion or anti-GPVI antibodies decreases neutrophil recruitment and activation, leading to reduced lung damage and hypoxia. Figure prepared with assistance from Diana Lim.

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