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血管紧张素转换酶抑制剂和血管扩张剂对原发性高血压患者肾功能曲线的不同影响。

Differential effects of ACE inhibitors and vasodilators on renal function curve in patients with primary hypertension.

作者信息

Fliser D, Nowack R, Wolf G, Ritz E

机构信息

Department of Internal Medicine, University of Heidelberg, Germany.

出版信息

Blood Press. 1993 Dec;2(4):296-300. doi: 10.3109/08037059309077171.

Abstract

OBJECTIVE

In experimental studies differential effects of antihypertensive agents on the renal function curve have been observed: in SHR captopril lowered the slope of the renal function curve, i.e. blood pressure (BP) became salt sensitive, whereas hydralazine shifted the curve without changing its slope. To evaluate whether ACE inhibitors and vasodilators have different effects on salt sensitivity of BP in humans, we compared the effect of the ACE inhibitor cilazapril and the vasodilator dihydralazine on the renal function curve in a randomized prospective single blind cross-over study.

DESIGN

Nine patients (1 f, 8 m, mean age 41 +/- 4 y) with mild to moderate primary hypertension were put on low (20 mmol/d) and on high salt diet (200 mmol/d). Drugs were given in random low salt+cilazapril, high salt+cilazapril; low salt+dihydralazine, high salt+dihydralazine; or in reverse order.

RESULTS

All antihypertensive interventions lowered BP, but the averaged posttreatment MAP was significantly (p < 0.02) lower with cilazapril on low salt intake (83.6 +/- 2.8 mmHg) than with all of the following: cilazapril on high salt intake (86.4 +/- 2.9 mmHg), dihydralazine on low (91.6 +/- 3.2 mmHg) and high salt (90.1 +/- 3.3 mmHg) intake. Probably as a result of sympathetic activation, average daily heart rate was higher after dihydralazine on low (72.9 +/- 2.9 b/min) and high salt intake (72.4 +/- 2.8 b/min) than after cilazapril on either salt intake (68.7 +/- 3.1 and 62.7 +/- 3.2 b/min).

CONCLUSIONS

The results document that BP reduction after acute ACE inhibition is a function of salt intake, i.e. with ACE inhibitor therapy, BP is "salt sensitive". In contrast, vasodilators of the dihydralazine type have similar antihypertensive effects on low and high salt intake. To the extent that the findings of this short-term study can be extrapolated to long-term effects they suggest that intrarenal mechanisms, i.e. resetting of the pressure-natriuresis relationship, are involved in the long-term antihypertensive action of ACE inhibitors.

摘要

目的

在实验研究中,已观察到抗高血压药物对肾功能曲线有不同影响:在自发性高血压大鼠(SHR)中,卡托普利降低了肾功能曲线的斜率,即血压(BP)变得对盐敏感,而肼屈嗪使曲线移位但不改变其斜率。为评估血管紧张素转换酶(ACE)抑制剂和血管扩张剂对人类血压盐敏感性是否有不同影响,我们在一项随机前瞻性单盲交叉研究中比较了ACE抑制剂西拉普利和血管扩张剂双肼屈嗪对肾功能曲线的影响。

设计

9例(1例女性,8例男性,平均年龄41±4岁)轻度至中度原发性高血压患者接受低(20 mmol/d)盐饮食和高盐(200 mmol/d)饮食。药物给药顺序为随机:低盐+西拉普利、高盐+西拉普利;低盐+双肼屈嗪、高盐+双肼屈嗪;或相反顺序。

结果

所有抗高血压干预措施均降低了血压,但低盐摄入时服用西拉普利后的平均治疗后平均动脉压(MAP)显著(p<0.02)低于以下所有情况:高盐摄入时服用西拉普利(86.4±2.9 mmHg)、低盐摄入时服用双肼屈嗪(91.6±3.2 mmHg)和高盐摄入时服用双肼屈嗪(90.1±3.3 mmHg)。可能由于交感神经激活,低盐摄入(72.9±2.9次/分钟)和高盐摄入(72.4±2.8次/分钟)时服用双肼屈嗪后的平均每日心率高于两种盐摄入情况下服用西拉普利后的心率(68.7±3.1次/分钟和62.7±3.2次/分钟)。

结论

结果表明急性ACE抑制后血压降低是盐摄入的函数,即采用ACE抑制剂治疗时,血压“对盐敏感”。相比之下,双肼屈嗪类血管扩张剂在低盐和高盐摄入时具有相似的抗高血压作用。就这项短期研究的结果可外推至长期效应而言,它们提示肾内机制,即压力-利钠关系的重新设定,参与了ACE抑制剂的长期抗高血压作用。

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