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用于合并肾功能损害的高血压患者的钙通道阻滞剂治疗:以伊拉地平为重点

Calcium-channel entry blocker therapy for hypertensive patients with concomitant renal impairment: a focus on isradipine.

作者信息

Frishman W H

机构信息

Department of Medicine, Albert Einstein College of Medicine/Montefiore Medical Center, Bronx, New York.

出版信息

J Clin Pharmacol. 1994 Dec;34(12):1164-72. doi: 10.1002/j.1552-4604.1994.tb04727.x.

Abstract

In the treatment of hypertension in renally impaired patients, normalization of blood pressure alone may not be sufficient to prevent significant morbidity to the kidneys. Treatment must reduce pressure in the renal vasculature, otherwise glomerular filtration rate and renal plasma flow will continue to deteriorate. Isradipine a dihydropyridine calcium-channel blocker, has been investigated as a suitable treatment in this setting. Isradipine maintains glomerular filtration rate, preserves or enhances renal plasma flow, decreases renal vascular resistance, maintains or reduces filtration fraction, and exerts a sustained natriuretic effect, all of which may enable isradipine to slow the rate of progression of renal deterioration. In addition, isradipine may decrease proteinuria and may decrease glomerular capillary pressure by dilating both the efferent and afferent arterioles. Unlike older calcium-channel blockers, isradipine exhibits minimal cardiodepressant activity and is not associated with any negative inotropic effects. It is metabolized in the liver and dosage adjustments may not be necessary when administered to patients with renal insufficiency. Isradipine has a favorable renal effect profile and also has several properties that meet the requirements of other patient populations where an extra measure of antihypertensive safety is required, such as diabetics, dialysis patients, and transplant recipients. Side effects with isradipine are usually mild and transient, occurring in a dose-dependent manner.

摘要

在治疗肾功能受损患者的高血压时,仅使血压正常化可能不足以预防对肾脏的显著损害。治疗必须降低肾血管系统的压力,否则肾小球滤过率和肾血浆流量将继续恶化。伊拉地平是一种二氢吡啶类钙通道阻滞剂,已被研究作为这种情况下的合适治疗方法。伊拉地平可维持肾小球滤过率,保持或增加肾血浆流量,降低肾血管阻力,维持或降低滤过分数,并产生持续的利钠作用,所有这些都可能使伊拉地平减缓肾脏恶化的速度。此外,伊拉地平可能会减少蛋白尿,并可通过扩张出球小动脉和入球小动脉来降低肾小球毛细血管压力。与 older 钙通道阻滞剂不同,伊拉地平表现出最小的心脏抑制活性,且与任何负性肌力作用无关。它在肝脏中代谢,给予肾功能不全患者时可能无需调整剂量。伊拉地平具有良好的肾脏效应特征,并且还具有一些特性,满足其他需要额外抗高血压安全性措施的患者群体的要求,如糖尿病患者、透析患者和移植受者。伊拉地平的副作用通常轻微且短暂,呈剂量依赖性发生。

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