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A comparative review of neutrophil extracellular traps in sepsis

机译:败血症中性粒细胞外细胞陷阱的比较研究

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Sepsis is the leading cause of critical illness and mortality in human beings and animals. Neutrophils are the primary effector cells of innate immunity during sepsis. Besides degranulation and phagocytosis, neutrophils also release neutrophil extracellular traps (NETs), composed of cell-free DNA, histones and antimicrobial proteins. Although NETs have protective roles in the initial stages of sepsis, excessive NET formation has been found to induce thrombosis and multiple organ failure in murine sepsis models. Since the discovery of NETs nearly a decade ago, many investigators have identified NETs in various species. However, many questions remain regarding the exact mechanisms and fate of neutrophils following NET formation. In humans and mice, platelet-neutrophil interactions via direct binding or soluble mediators seem to play an important role in mediating NET formation during sepsis. Preliminary data suggest that these interactions may be species dependent. Regardless of these differences, there is increasing evidence in human and veterinary medicine suggesting that NETs play a crucial role in the pathogenesis of intravascular thrombosis and multiple organ failure in sepsis. Because the outcome of sepsis is highly dependent on early recognition and intervention, detection of NETs or NET components can aid in the diagnosis of sepsis in humans and veterinary species. In addition, the use of novel therapies such as deoxyribonuclease and non-anticoagulant heparin to target NET components shows promising results in murine septic models. Much work is needed in translating these NET-targeting therapies to clinical practice.
机译:败血症是人类和动物严重疾病和死亡的主要原因。中性粒细胞是败血症过程中先天免疫的主要效应细胞。除了脱粒和吞噬作用,中性粒细胞还释放中性粒细胞胞外陷阱(NETs),该陷阱由无细胞的DNA,组蛋白和抗菌蛋白组成。尽管NET在脓毒症的初始阶段起保护作用,但已发现过量的NET形成可在小鼠败血症模型中诱发血栓形成和多器官功能衰竭。自从大约十年前发现NET以来,许多研究人员已经鉴定出各种物种的NET。然而,NET形成后中性粒细胞的确切机制和命运仍然存在许多问题。在人类和小鼠中,通过直接结合或可溶性介导的血小板-中性粒细胞相互作用似乎在败血症期间介导NET形成中起重要作用。初步数据表明,这些相互作用可能与物种有关。无论这些差异如何,在人类和兽医学中越来越多的证据表明NET在脓毒症的血管内血栓形成和多器官功能衰竭的发病机理中起着至关重要的作用。由于败血症的结果高度依赖于早期识别和干预,因此对NETs或NET组件的检测可以帮助诊断人类和兽医类败血症。此外,在鼠类败血病模型中使用新型疗法(如脱氧核糖核酸酶和非抗凝肝素)靶向NET成分显示出令人鼓舞的结果。将这些以NET为目标的疗法转化为临床实践需要大量工作。

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