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伊洛前列素可改善缺血后肺再灌注损伤,并维持适当的肺内皮素-1平衡。

Iloprost ameliorates post-ischemic lung reperfusion injury and maintains an appropriate pulmonary ET-1 balance.

作者信息

Kawashima Masahiro, Nakamura Takayuki, Schneider Sven, Vollmar Brigitte, Lausberg Henning F, Bauer Michael, Menger Michael D, Schäfers Hans-Joachim

机构信息

Department of Thoracic and Cardiovascular Surgery, University of Saarland, Homburg/Saar, Germany.

出版信息

J Heart Lung Transplant. 2003 Jul;22(7):794-801. doi: 10.1016/s1053-2498(02)00646-0.

Abstract

BACKGROUND

Ischemia-reperfusion (I/R) injury of the lung involves increased pulmonary vascular resistance. Prostaglandins are thought to have a beneficial effect in lung transplantation, but their mechanism in I/R injury is unknown. We investigated whether iloprost, a stable prostacyclin analogue, prevents I/R-associated pulmonary vascular dysfunction and whether it affects endothelin-1 (ET-1) balance.

METHODS

In an isolated blood-perfusion model, we subjected lungs of Lewis rats to 45 minutes of ischemia at 37 degrees C and randomly allocated the lungs to 3 groups (n = 6 each): iloprost (33.3 nmol/liter) added to the perfusate before ischemia and reperfusion (ILO+IR), iloprost (33.3 nmol/liter) given only before reperfusion (ILO+R), and controls without iloprost treatment (ILO-).

RESULTS

Reperfusion induced marked pulmonary edema in non-treated controls (ILO-), which was attenuated in ILO+R lungs and completely prevented in ILO+IR lungs. At 60 minutes reperfusion, arterial oxygen tension was significantly greater in both ILO+R and ILO+IR lungs compared with ILO- controls. Mean pulmonary artery pressure and pulmonary vascular resistance were slightly decreased in the ILO+R and significantly decreased in the ILO+IR group compared with the ILO- controls. Plasma levels of big ET-1, measured in both afferent and efferent blood, showed that I/R results in increased pulmonary venous levels of big ET-1. Interestingly, the increased venoarterial ET-1 gradient in ILO- lungs decreased significantly in the ILO+IR group.

CONCLUSIONS

We demonstrated in an isolated lung perfusion model that iloprost ameliorates post-ischemic lung reperfusion injury and maintains an appropriate pulmonary ET-1 balance.

摘要

背景

肺缺血-再灌注(I/R)损伤涉及肺血管阻力增加。前列腺素被认为在肺移植中具有有益作用,但其在I/R损伤中的机制尚不清楚。我们研究了稳定的前列环素类似物伊洛前列素是否能预防I/R相关的肺血管功能障碍以及它是否影响内皮素-1(ET-1)平衡。

方法

在一个离体血液灌注模型中,我们将Lewis大鼠的肺在37℃下进行45分钟的缺血处理,然后将肺随机分为3组(每组n = 6):在缺血和再灌注前向灌注液中添加伊洛前列素(33.3 nmol/升)(ILO+IR),仅在再灌注前给予伊洛前列素(33.3 nmol/升)(ILO+R),以及未用伊洛前列素处理的对照组(ILO-)。

结果

再灌注在未处理的对照组(ILO-)中引起明显的肺水肿,在ILO+R组的肺中减轻,在ILO+IR组的肺中完全预防。在再灌注60分钟时,与ILO-对照组相比,ILO+R组和ILO+IR组的动脉血氧分压均显著更高。与ILO-对照组相比,ILO+R组的平均肺动脉压和肺血管阻力略有降低,ILO+IR组则显著降低。在传入和传出血液中测量的大ET-1血浆水平表明,I/R导致肺静脉中大ET-1水平升高。有趣的是,ILO-组肺中增加的静脉-动脉ET-1梯度在ILO+IR组中显著降低。

结论

我们在一个离体肺灌注模型中证明,伊洛前列素可改善缺血后肺再灌注损伤并维持适当的肺ET-1平衡。

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