Lefer A M, Lefer D J
Department of Physiology, Jefferson Medical College, Thomas Jefferson University, Philadelphia, Pennsylvania 19107, USA.
Am J Physiol. 1999 Mar;276(3):G572-5. doi: 10.1152/ajpgi.1999.276.3.G572.
This article examines the evidence for nitric oxide (NO) as a protective agent in splanchnic ischemia-reperfusion and other forms of acute intestinal inflammation. Four major points emerge from this body of data. First, acute intestinal inflammation results in an early (i.e., <5 min) and severe decrease in endothelium-derived NO. Thus the early trigger event in this condition is a functional loss of NO. Second, administration of exogenous NO, NO donors, or NO precursors ameliorate splanchnic ischemia-reperfusion and other forms of acute intestinal inflammation (i.e., splanchnic trauma). These beneficial effects occur at physiological levels of NO when given early in the course of the inflammatory state. Third, blockade of nitric oxide synthase (NOS) or gene deletion of NOS exacerbates intestinal inflammation. Fourth, there are a variety of signaling mechanisms that may mediate the protective effect of NO.
本文探讨了一氧化氮(NO)作为内脏缺血再灌注及其他形式急性肠道炎症保护剂的证据。从这组数据中得出四个要点。首先,急性肠道炎症会导致内皮源性NO早期(即<5分钟)且严重减少。因此,这种情况下的早期触发事件是NO功能丧失。其次,给予外源性NO、NO供体或NO前体可改善内脏缺血再灌注及其他形式的急性肠道炎症(即内脏创伤)。在炎症状态早期给予时,这些有益作用在生理水平的NO时出现。第三,一氧化氮合酶(NOS)的阻断或NOS基因缺失会加剧肠道炎症。第四,存在多种信号传导机制可能介导NO的保护作用。