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人类左心室功能的旁分泌性冠状动脉内皮调控

Paracrine coronary endothelial control of left ventricular function in humans.

作者信息

Paulus W J, Vantrimpont P J, Shah A M

机构信息

Cardiovascular Center, OLV Ziekenhuis, Aalst, Belgium.

出版信息

Circulation. 1995 Oct 15;92(8):2119-26. doi: 10.1161/01.cir.92.8.2119.

Abstract

BACKGROUND

Similar to endothelial modulation of vascular tone, myocardial contraction may be modulated by cardioactive agents released from the coronary endothelium. To investigate such modulation in humans, we performed invasive assessment of left ventricular (LV) function before, during, and after bicoronary infusion of substance P, which releases nitric oxide from the endothelium.

METHODS AND RESULTS

Eight healthy subjects were investigated during diagnostic coronary angiography and eight transplant recipients during annual catheterization. Tip-micromanometer LV pressure was recorded before, during, and after bicoronary (n = 16) and right atrial (n = 14) infusion of substance P (20 pmol/min). LV angiograms (n = 11) were obtained before and at the end of the substance P infusion. At the end of the intracoronary substance P infusion, we observed (1) a fall in LV peak systolic pressure from 147 +/- 16 to 139 +/- 15 mm Hg (P < .01) in healthy subjects and from 147 +/- 25 to 141 +/- 22 mmHg (P < .05) in transplant recipients; (2) a downward and rightward shift of the average LV end-systolic pressure-volume point consistent with depressed systolic performance; and (3) a rise in LV end-diastolic volume at comparable end-diastolic pressure, consistent with increased end-diastolic distensibility. Five minutes after the substance P infusion, LV peak systolic pressure was higher than at baseline in healthy subjects (154 +/- 18 mm Hg; P < .05). Right atrial infusion of substance P did not reproduce these changes.

CONCLUSIONS

Bicoronary infusion of substance P modulates LV function in humans, probably through paracrine myocardial action of cardioactive agents released from the coronary endothelium.

摘要

背景

与血管内皮对血管张力的调节类似,心肌收缩可能受到冠状动脉内皮释放的心脏活性物质的调节。为了研究人类的这种调节作用,我们在双冠状动脉内输注P物质(该物质可从内皮释放一氧化氮)之前、期间和之后,对左心室(LV)功能进行了有创评估。

方法与结果

在诊断性冠状动脉造影期间对8名健康受试者进行了研究,在年度导管插入术期间对8名移植受者进行了研究。在双冠状动脉(n = 16)和右心房(n = 14)输注P物质(20 pmol/分钟)之前、期间和之后,记录尖端微测压计的左心室压力。在P物质输注前和输注结束时获取左心室血管造影(n = 11)。在冠状动脉内P物质输注结束时,我们观察到:(1)健康受试者的左心室收缩压峰值从147±16降至139±15 mmHg(P <.01),移植受者从147±25降至141±22 mmHg(P <.05);(2)平均左心室收缩末期压力-容积点向下和向右移位,这与收缩功能降低一致;(3)在可比的舒张末期压力下,左心室舒张末期容积增加,这与舒张末期扩张性增加一致。在P物质输注后5分钟,健康受试者的左心室收缩压峰值高于基线(154±18 mmHg;P <.05)。右心房输注P物质未重现这些变化。

结论

双冠状动脉内输注P物质可调节人类的左心室功能,可能是通过冠状动脉内皮释放的心脏活性物质的旁分泌心肌作用实现的。

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