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首页> 外文期刊>Acta Pharmacologica Sinica >Effects of endothelin and nitric oxide on organ injury, mesenteric ischemia, and survival in experimental models of septic shock
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Effects of endothelin and nitric oxide on organ injury, mesenteric ischemia, and survival in experimental models of septic shock

机译:败血性休克实验模型中内皮素和一氧化氮对器官损伤,肠系膜缺血和存活的影响

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摘要

The development of potent drugs to treat cardiopulmonary failure in sepsis, such as antibiotics and new immunomodulatory therapeutic approaches have not prevented sepsis from being a major health problem. Dysfunction of the vascular endothelium is an early event in septic shock. The recognition of endothelium-derived substances, such as nitric oxide and endothelin, important mediators of systemic inflammatory response syndrome, led to the proposal that pharmacological inhibition of nitric oxide and endothelin production could represent a useful strategy in the treatment of septic shock. Splanchnic ischemia and translocation of endotoxin from the gut to the circulation contributes significantly to the high mortality rate in sepsis-related syndromes. This vasoconstriction in the splanchnic circulation can be partially blocked by inducible nitric oxide synthase inhibitor aminoguanidine or endothelin receptor antagonist bosentan in experimental models of septic shock. It can be suggested that endothelin and nitric oxide may affect survival. Although septic shock is a highly complex pathophysiological state, the course of septic shock has different phases with different characteristics which need different (special) treatment strategy. The inhibition of nitric oxide production during hyperdynamic, earlier phase of sepsis combined with the blockade of endothelin receptors at a later stage during the hypodynamic, late phase appears to be a novel promising strategy for the therapy of septic shock. The aim of this review is to discuss the role of nitric oxide and endothelin in sepsis and the potential therapeutic implications of blockade of nitric oxide and endothelin as a target in treatment of human septic shock. Briefly the importance of timing of intervention is also emphasized.
机译:开发治疗脓毒症心肺衰竭的有效药物,例如抗生素和新的免疫调节治疗方法,并未阻止脓毒症成为主要的健康问题。血管内皮功能障碍是败血性休克的早期事件。认识到内皮源性物质如一氧化氮和内皮素是全身性炎症反应综合征的重要介质,因此提出了这样的建议,即药理抑制一氧化氮和内皮素的产生可以代表治疗脓毒性休克的有用策略。内脏缺血和内毒素从肠道转移到血液循环显着促进败血症相关综合征的高死亡率。在败血性休克的实验模型中,可诱导的一氧化氮合酶抑制剂氨基胍或内皮素受体拮抗剂波生坦可部分阻止内脏循环中的这种血管收缩。提示内皮素和一氧化氮可能会影响生存。尽管败血性休克是高度复杂的病理生理状态,但是败血性休克的病程具有不同的阶段,具有不同的特征,需要不同的(特殊)治疗策略。在脓毒症的高动力性早期阶段抑制一氧化氮的产生,在低动力性晚期阶段抑制内皮素受体的结合,似乎是治疗脓毒性休克的一种新的有前途的策略。这篇综述的目的是讨论一氧化氮和内皮素在脓毒症中的作用以及一氧化氮和内皮素的阻断作为治疗人类败血性休克的靶标的潜在治疗意义。简要地,还强调了干预时机的重要性。

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