正常和慢性缺氧大鼠肺循环的内皮调控
Endothelial control of the pulmonary circulation in normal and chronically hypoxic rats.
作者信息
Barer G, Emery C, Stewart A, Bee D, Howard P
机构信息
Department of Medicine and Pharmacology, University of Sheffield, Royal Hallamshire Hospital.
出版信息
J Physiol. 1993 Apr;463:1-16. doi: 10.1113/jphysiol.1993.sp019581.
Abstract
- The effect of blockade of nitric oxide synthesis in pulmonary endothelium by two L-arginine analogues was tested in isolated blood-perfused lungs of normal rats and rats exposed chronically to 10% O2. 2. In both groups of rats the analogues (N-monomethyl-L-arginine (L-NMMA) and N-nitro-L-arginine methyl ester (L-NAME)) enhanced hypoxic vasoconstriction. In normal rats, with rare exceptions, these analogues had little or no effect on pulmonary artery pressure (Ppa) at constant blood flow during normoxia. However, chronically hypoxic rats have pulmonary hypertension and in these rats the analogues always raised Ppa; the rise in Ppa after L-NMMA but not L-NAME could be partially reversed by L-arginine. L-NAME was more potent than L-NMMA. 3. To see whether the difference between rat groups was due to the high Ppa in chronically hypoxic rats, in control rats we raised Ppa passively by lung inflation to values higher than found in chronically hypoxic rats. L-NAME did not alter the effects of lung inflation on Ppa. 4. Ppa was also raised passively by plotting pressure-flow lines up to high flow rates; the lines were changed minimally by both analogues in control rats but in chronically hypoxic rats the lines were raised to higher pressures and steepened substantially. 5. In control rats, during vasoconstriction caused by hypoxia, endothelin 1 and almitrine, L-NAME caused further rises in pressure. We conclude that a stimulus for nitric oxide release in control rats is the narrowing of vessels caused by vasoconstriction rather than passive increases in intravascular pressure. 6. In chronically hypoxic rats arterioles are narrowed by growth of new muscle and there is some muscle tone even in normoxia. Thus narrowing of the vascular lumen is the stimulus common to both groups of rats which leads to nitric oxide synthesis and attenuation of Ppa by a negative feedback process. Narrowing is associated with a large increase in shear stress due to two factors; the pressure drop along a vessel segment is increased and the surface area of the lining of the affected segment is decreased. 7. Atrial natriuretic peptide caused dose-dependent pulmonary vasodilation in both rat groups but had a greater effect in chronically hypoxic rats. The action persisted and was enhanced after blockade of NO synthesis.
摘要
- 在正常大鼠以及长期暴露于10%氧气环境的大鼠的离体血液灌注肺中,测试了两种L-精氨酸类似物对肺内皮细胞一氧化氮合成的阻断作用。2. 在两组大鼠中,这些类似物(N-单甲基-L-精氨酸(L-NMMA)和N-硝基-L-精氨酸甲酯(L-NAME))均增强了缺氧性血管收缩。在正常大鼠中,除极少数情况外,这些类似物在常氧状态下恒定血流时对肺动脉压(Ppa)几乎没有影响或无影响。然而,长期缺氧的大鼠患有肺动脉高压,在这些大鼠中,这些类似物总是会升高Ppa;L-NMMA后Ppa的升高但L-NAME后不会,L-精氨酸可部分逆转L-NMMA引起的Ppa升高。L-NAME比L-NMMA更有效。3. 为了探究大鼠组之间的差异是否归因于长期缺氧大鼠的高Ppa,在对照大鼠中,我们通过肺膨胀被动地将Ppa升高至高于长期缺氧大鼠所测得的值。L-NAME并未改变肺膨胀对Ppa的影响。4. 通过绘制直至高流速的压力-流量曲线也可被动地升高Ppa;在对照大鼠中,两种类似物对曲线的改变极小,但在长期缺氧大鼠中,曲线升高至更高压力且显著变陡。5. 在对照大鼠中,在由缺氧、内皮素-1和阿米三嗪引起的血管收缩过程中,L-NAME导致压力进一步升高。我们得出结论,对照大鼠中一氧化氮释放的刺激因素是血管收缩引起的血管狭窄,而非血管内压力的被动升高。6. 在长期缺氧的大鼠中,小动脉因新肌肉生长而变窄,即使在常氧状态下也存在一定的肌张力。因此,血管腔狭窄是两组大鼠共同的刺激因素,其通过负反馈过程导致一氧化氮合成并使Ppa降低。狭窄与剪切应力的大幅增加有关,这是由于两个因素;沿血管段的压力降增加以及受影响段内衬的表面积减小。7. 心房利钠肽在两组大鼠中均引起剂量依赖性的肺血管舒张,但在长期缺氧大鼠中作用更强。在一氧化氮合成被阻断后,该作用持续存在且增强。
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