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Platelet-activating factor and platelet-activating factor antagonists in acute pancreatitis.

机译:急性胰腺炎中的血小板活化因子和血小板活化因子拮抗剂。

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INTRODUCTION: Acute pancreatitis causes platelet-activating factor (PAF) to be released which induces systemic effects that contribute to circulatory disturbances and multiple organ failure. PAF has also been implicated as a key mediator in the progression of severe acute pancreatitis, which can lead to complications and unacceptably high mortality rates. MODE OF ACTION OF PAF IN ACUTE PANCREATITIS: Synthesis of PAF is sensitive to biologically active mediators seen in many inflammatory processes. PAF significantly potentiates pancreatic tissue damage; it causes serum amylase and lipase levels to rise significantly, causes scattered haemorrhages and may serve as a primary mediator of inflammation. PAF ANTAGONISTS: Several classes of compounds show significant PAF antagonisms, and all have shown significant local and systemic effects to reduce inflammatory changes. Only lexipafant, however, has been studied in human acute pancreatitis. Lexipafant specifically binds to the PAF receptor and is more potent than other PAF antagonists. In clinical trials lexipafant reduces organ failure and suppresses some aspects of the inflammatory response. CONCLUSION: Our understanding of the pathology of systemic complications, and of a central role of PAF in mediating an inappropriate inflammatory response has improved in recent years. Confirmation of clinical findings with lexipafant will indicate an effective new therapy for the treatment of severe acute pancreatitis.
机译:简介:急性胰腺炎会导致血小板活化因子(PAF)释放,从而诱发全身性作用,从而导致循环系统紊乱和多器官功能衰竭。 PAF还被认为是严重急性胰腺炎进展中的关键介质,它可能导致并发症和高死亡率。 PAF在急性胰腺炎中的作用模式:PAF的合成对许多炎症过程中观察到的生物活性介质敏感。 PAF可显着增强胰腺组织损伤。它会导致血清淀粉酶和脂肪酶水平显着升高,引起零星出血,并可能是炎症的主要介质。 PAF拮抗剂:几类化合物显示出显着的PAF拮抗作用,并且都显示出显着的局部和全身作用以减少炎症变化。然而,在人类急性胰腺炎中仅研究了立哌卡芬。 Lexipafant特异性结合PAF受体,并且比其他PAF拮抗剂更有效。在临床试验中,Lexipafant可减少器官衰竭并抑制炎症反应的某些方面。结论:近年来,我们对全身并发症的病理学以及PAF在介导不适当的炎症反应中的重要作用的了解有所提高。 Lexipafant的临床发现的确认将指示一种用于治疗严重急性胰腺炎的有效新疗法。

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