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大鼠骨骼肌原位小动脉直径的血流依赖性调节:内皮源性舒张因子和前列腺素的作用。

Flow-dependent regulation of arteriolar diameter in rat skeletal muscle in situ: role of endothelium-derived relaxing factor and prostanoids.

作者信息

Friebel M, Klotz K F, Ley K, Gaehtgens P, Pries A R

机构信息

Department of Physiology, Freie Universität Berlin, Germany.

出版信息

J Physiol. 1995 Mar 15;483 ( Pt 3)(Pt 3):715-26. doi: 10.1113/jphysiol.1995.sp020616.

Abstract
  1. Arteriolar diameter in the resting rat spinotrapezius muscle was studied by intravital video microscopy before and after blockade of the L-arginine-EDRF (NG-nitro-L-arginine, L-NNA) or the cyclo-oxygenase-prostacyclin (indomethacin) pathway. Blockade of either pathway leads to a decrease of arteriolar diameter of 25-40%, while the combined blockade of both results in vasoconstriction of 50-60%. 2. Alteration of blood flow velocity elicited by partial micropipette occlusion induces corresponding changes of vessel diameter. The flow-dependent diameter response is reduced by about 80% by L-NNA. By contrast, blockade of prostanoid production shows no significant influence on vessel response to blood flow alteration in the range tested. 3. Transient overshooting vasodilatation is seen for about 1 min following the sudden restoration of flow velocity subsequent to occlusion. In contrast to the initial phase of this response, the late phase is blocked by L-NNA. 4. The findings suggest that basal release of endothelium-derived relaxing factor (EDRF) and prostanoids leads to additive and independent dilator effects, and that flow-dependent diameter changes are primarily mediated by EDRF. 5. If present data are compared with literature reports, it appears that arterial flow sensitivity is most pronounced in the smallest vessels. In such vessels, flow-dependent dilatation will amplify even small changes of volume flow by more than four times.
摘要
  1. 在阻断L-精氨酸-内皮舒张因子(NG-硝基-L-精氨酸,L-NNA)或环氧化酶-前列环素(吲哚美辛)途径之前和之后,通过活体视频显微镜研究了静息大鼠斜方肌中的小动脉直径。阻断任一途径都会导致小动脉直径减小25%-40%,而同时阻断两者则会导致50%-60%的血管收缩。2. 部分微量移液器阻塞引起的血流速度改变会导致相应的血管直径变化。L-NNA可使血流依赖性直径反应降低约80%。相比之下,在测试范围内,阻断前列腺素生成对血管对血流改变的反应没有显著影响。3. 在阻塞后血流速度突然恢复后的约1分钟内可见短暂的过度血管舒张。与该反应的初始阶段不同,后期阶段被L-NNA阻断。4. 这些发现表明,内皮源性舒张因子(EDRF)和前列腺素的基础释放会产生累加且独立的舒张作用,并且血流依赖性直径变化主要由EDRF介导。5. 如果将目前的数据与文献报道进行比较,似乎动脉血流敏感性在最小的血管中最为明显。在这类血管中,血流依赖性舒张会使体积流量的微小变化放大四倍以上。

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