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通过抑制血管紧张素转换酶降低蛋白尿

Reduction of proteinuria by angiotensin converting enzyme inhibition.

作者信息

Heeg J E, de Jong P E, van der Hem G K, de Zeeuw D

出版信息

Kidney Int. 1987 Jul;32(1):78-83. doi: 10.1038/ki.1987.174.

Abstract

The effects of the angiotensin converting enzyme (ACE) inhibitor lisinopril on blood pressure, proteinuria and renal hemodynamics were evaluated in 13 patients with renal disease of different origin. A comparison was made with the effects of conventional antihypertensive therapy. Both drug regimens significantly lowered blood pressure, while only after 12 weeks of treatment with lisinopril, blood pressure was significantly lower than during conventional therapy. Lisinopril reduced proteinuria (by 61 +/- 40%), whereas conventional therapy had no significant effect on protein excretion. During the first eight weeks of treatment with lisinopril, there was a comparable degree of blood pressure reduction with both treatment regimens, whereas urinary protein loss was significantly less during ACE inhibition. There was only a nearly-significant positive correlation between the fall in proteinuria during lisinopril and the concomitant decrease in mean arterial pressure. Glomerular filtration rate decreased from 26.3 +/- 11.6 to 20.6 +/- 9.4 ml/min during treatment with lisinopril. This decrease was not correlated with the fall in proteinuria. A significant positive correlation existed between the fall in urinary protein excretion and both the decrease in overall renal vascular resistance, and the fall in filtration fraction. Although blood pressure lowering by itself could contribute to the antiproteinuric effect of lisinopril, our results suggest that this effect of ACE inhibition is also due to efferent (postglomerular) vasodilation. We conclude that the ACE inhibitor lisinopril effectively reduces blood pressure and proteinuria in renal disease. The latter effect is not only the result of a lower blood pressure, but is probably also due to a fall in intraglomerular capillary pressure.

摘要

在13例不同病因的肾病患者中评估了血管紧张素转换酶(ACE)抑制剂赖诺普利对血压、蛋白尿和肾血流动力学的影响。并与传统抗高血压治疗的效果进行了比较。两种药物治疗方案均能显著降低血压,但仅在使用赖诺普利治疗12周后,血压才显著低于传统治疗期间。赖诺普利可降低蛋白尿(降低61±40%),而传统治疗对尿蛋白排泄无显著影响。在使用赖诺普利治疗的前八周,两种治疗方案的血压降低程度相当,而在ACE抑制期间尿蛋白丢失显著减少。赖诺普利治疗期间蛋白尿的下降与平均动脉压的相应降低之间仅存在近乎显著的正相关。在使用赖诺普利治疗期间,肾小球滤过率从26.3±11.6降至20.6±9.4 ml/min。这种下降与蛋白尿的下降无关。尿蛋白排泄的下降与总肾血管阻力的降低以及滤过分数的下降之间存在显著的正相关。尽管血压降低本身可能有助于赖诺普利的抗蛋白尿作用,但我们的结果表明,ACE抑制的这种作用也归因于出球(肾小球后)血管舒张。我们得出结论,ACE抑制剂赖诺普利可有效降低肾病患者的血压和蛋白尿。后一种作用不仅是血压降低的结果,还可能归因于肾小球内毛细血管压力的下降。

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