The effect of neutrophil extracellular traps(NETs)on promoting intravascular microthrombi formation and exacerbating the severity of sepsis in patients has gained extensive attention.However,in sepsis,the mechanisms and key signaling molecules mediating NET formation during direct interactions of endothelial cells and neutrophils still need further explored.Herein,we utilized lipoteichoic acid(LTA),a component shared by Gram-positive bacteria,to induce NET extrusion from neutrophils firmly adhered to the glass slides coated with intercellular adhesion molecule-1(ICAM-1).We also used Sytox green to label NET-DNA and Flou-4 AM as the intracellular Ca2+signaling indicator to observe the NET formation and fluctuation of Ca2+signaling.Our results illustrated that LTA was able to induce NET release from neutrophils firmly attached to ICAM-1-coated glass slides,and the process was time-dependent.In addition,our study indicated that LTA-induced NET release by neutrophils stably adhered to ICAM-1 depended on Ca2+signaling but not intracellular reactive oxygen species(ROS).This study reveals NET formation mediated by direct interactions between endothelial ICAM-1 and neutrophils under LTA stimulation and key signaling molecules involved,providing the theoretical basis for medicine development and clinical treatment for related diseases.
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