同型半胱氨酸对离体大鼠股动脉急性作用的转导机制分析。

Miroslav Radenković, D Djurić, R Janković, M Prostran
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引用次数: 4

摘要

本研究旨在探讨100 μM同型半胱氨酸(Hcy)单次应用于离体大鼠股动脉(RFA)环的传导机制;观察100 μM Hcy孵育60 min后,单次施加100 μM Hcy是否会改变苯肾上腺素(Phe)的收缩作用,或相反改变乙酰胆碱(ACh)或缓动素(BK)的松弛作用;最后观察100 μM Hcy孵育24 h后血管壁的形态学变化。Hcy产生完整RFA的收缩反应,内皮剥脱后RFA的收缩反应增加,而乌拉地尔(α1受体阻滞剂)、硝苯地平(电压门控l型ca++通道阻滞剂)或吲哚美辛(环加氧酶抑制剂)的收缩反应降低。单次加入Hcy后,Phe引起的初始RFA收缩进一步增加,而预孵育乌阿因(Na+/K+- atp酶抑制剂)时则没有这种情况。经60 min的Hcy孵育后,ACh和BK的松弛作用不变,具有等效和等效性。将RFA环与Hcy一起孵育24小时,可导致血管内皮受损,表现为内皮细胞的轻微或更明显的中断。
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The analysis of transduction mechanisms associated with an acute action of homocysteine on isolated rat femoral artery.

The present study was undertaken in order to examine transduction mechanism involved in the single application of 100 μM homocysteine (Hcy) on isolated rat femoral artery (RFA) rings equilibrated on the basal tone; to establish if a single application of 100 μM Hcy alters contractile effect of phenylephrine (Phe), or oppositely the relaxant effect of acetylcholine (ACh) or bradykinin (BK) after 60-min-long incubation of 100 μM Hcy; and finally to identify morphological changes on the vascular wall after a 24-h-long incubation of 100 μM Hcy. Hcy produced contractile response of intact RFA, which was increased after endothelial denudation, while decreased by urapidil (an α1 receptor blocker), nifedipine (a voltage-gated L-type Ca++ channel blocker) or indomethacin (a cyclooxygenase inhibitor). The initial RFA contraction evoked by Phe was further increased by the single addition of Hcy, which was not the case when ouabain (an inhibitor of Na+/K+-ATPase) was preincubated. After 60-min-long incubation of Hcy relaxant actions of ACh and BK were unaltered, equieffective and equipotent. A 24-h-long incubation of RFA rings with Hcy produced an impairment of vascular endothelium, expressed as a minor or more pronounced interruption of endothelial cells.

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来源期刊
Acta physiologica Hungarica
Acta physiologica Hungarica 医学-生理学
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