Eppinger M J, Ward P A, Jones M L, Bolling S F, Deeb G M
Section of Thoracic Surgery, University of Michigan Medical Center, Ann Arbor, USA.
Ann Thorac Surg. 1995 Nov;60(5):1169-75; discussion 1176. doi: 10.1016/0003-4975(95)00697-J.
Inhaled nitric oxide (.NO) has been found to be a potent pulmonary vasodilator. We assessed whether .NO, through this function or others, could alleviate lung reperfusion injury.
Rats underwent thoracotomy, with clamps used to create left lung ischemia. After 90 minutes of ischemia, clamps were released, permitting reperfusion for either 30 minutes or 4 hours. Additional animals received inhaled .NO via the ventilator to determine its effects on reperfusion injury.
Lung injury, measured by increased vascular permeability using iodine-125-labeled bovine serum albumin leakage, was significantly increased in ischemic-reperfused animals compared with time-matched shams not undergoing ischemia. Inhaled .NO delivered at the start of reperfusion worsened injury at 30 minutes but was protective at 4 hours. The increased injury could be avoided either by delaying .NO for 10 minutes or by treating the animals with superoxide dismutase before reperfusion. .NO reversed postischemic pulmonary hypoperfusion at 4 hours, as measured by labeled microspheres. Lung neutrophil content was significantly reduced at 4 hours in .NO-treated animals.
.NO is toxic early in reperfusion, due to its interaction with superoxide, but is protective at 4 hours of reperfusion, due to reversal of postischemic lung hypoperfusion and reduction of lung neutrophil sequestration.
吸入一氧化氮(.NO)已被发现是一种强效的肺血管扩张剂。我们评估了.NO是否通过该功能或其他功能来减轻肺再灌注损伤。
对大鼠进行开胸手术,用夹子造成左肺缺血。缺血90分钟后,松开夹子,使肺再灌注30分钟或4小时。另外的动物通过呼吸机吸入.NO,以确定其对再灌注损伤的影响。
与未经历缺血的时间匹配的假手术组相比,缺血再灌注动物中,通过使用碘-125标记的牛血清白蛋白渗漏来测量的血管通透性增加所反映的肺损伤显著增加。在再灌注开始时吸入.NO在30分钟时会加重损伤,但在4小时时具有保护作用。通过将.NO延迟10分钟或在再灌注前用超氧化物歧化酶治疗动物,可以避免损伤增加。通过标记微球测量,.NO在4小时时逆转了缺血后肺灌注不足。在接受.NO治疗的动物中,4小时时肺中性粒细胞含量显著降低。
.NO在再灌注早期具有毒性,这是由于其与超氧化物的相互作用,但在再灌注4小时时具有保护作用,这是由于逆转了缺血后肺灌注不足并减少了肺中性粒细胞的滞留。
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