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阻断肾素-血管紧张素系统对人体钠排泄的影响。

Effects of interrupting the renin-angiotensin system on sodium excretion in man.

作者信息

Brown J

机构信息

Department of Clinical Pharmacology, Royal Postgraduate Medical School, London.

出版信息

J Physiol. 1988 Jan;395:17-40. doi: 10.1113/jphysiol.1988.sp016906.

Abstract
  1. Twelve normal volunteers were studied on 2 separate days, having taken a range of diets providing 50-300 mmol sodium per day for 3 days and having been dehydrated overnight. Each volunteer received a background intravenous infusion of arginine vasopressin (5 x 10(-7) i.u. kg-1 min-1) on both days, and also received 6 mg captopril orally on one day and a placebo tablet on the other. The ensuing changes in arterial pressure, and in urinary solute and solute-free water excretion were recorded. 2. Captopril did not significantly alter arterial pressure. It increased the rate of excretion of sodium but not of potassium, and it did not significantly change urinary osmolality or creatinine clearance. 3. Captopril increased the rate of solute-free water reabsorption and did so in direct proportion to its effect of increasing sodium excretion. 4. A further twelve normal, dehydrated volunteers on free diets were studied on each of 2 days, after taking 500 mg lithium carbonate on the previous evening. On each day, they also received a loading dose and maintenance infusion of inulin. On one day they received 50 mg captopril orally, and, on the other, they received a placebo tablet. The arterial pressure, urinary excretion of electrolytes, and inulin clearance were recorded. 5. Captopril increased the rates of excretion of sodium, lithium and potassium, but there were no significant changes in inulin clearance or arterial pressure. 6. The natriuretic effect of captopril in either group of twelve volunteers was not significantly less in those volunteers who were already excreting more sodium, at least over the range of dietary sodium loading to which the volunteers were subjected. 7. Six normal volunteers were studied on a further 2 days, having taken a diet supplying 30 mmol sodium per day for 3 days and being dehydrated overnight. Each volunteer received a background intravenous infusion of arginine vasopressin (5 x 10(-7) i.u. kg-1 min-1) on both days and also received an intravenous infusion of saralasin acetate (50 ng kg-1 min-1) plus carrier on one day and carrier alone on the other. The ensuing changes in arterial pressure, and in urinary solute and solute-free water excretion were recorded. 8. There was a small but significant fall in systolic arterial pressure during the infusion of saralasin.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 12名正常志愿者在两个不同日期接受研究。他们连续3天摄入一系列每天提供50 - 300毫摩尔钠的饮食,并在前一晚进行脱水。在这两天里,每名志愿者均接受背景静脉输注精氨酸加压素(5×10⁻⁷国际单位/千克·分钟),且一天口服6毫克卡托普利,另一天口服安慰剂片。记录随后动脉压、尿溶质及无溶质水排泄的变化。2. 卡托普利未显著改变动脉压。它增加了钠的排泄率,但未增加钾的排泄率,且未显著改变尿渗透压或肌酐清除率。3. 卡托普利增加了无溶质水的重吸收率,且与其增加钠排泄的作用成正比。4. 另外12名正常、脱水且自由饮食的志愿者在前一晚服用500毫克碳酸锂后,在两个不同日期分别接受研究。每天他们还接受菊粉的负荷剂量及维持输注。一天口服50毫克卡托普利,另一天口服安慰剂片。记录动脉压、电解质的尿排泄及菊粉清除率。5. 卡托普利增加了钠、锂和钾的排泄率,但菊粉清除率或动脉压无显著变化。6. 在两组各12名志愿者中,至少在志愿者所接受的饮食钠负荷范围内,已排泄较多钠的志愿者中,卡托普利的利钠作用并无显著降低。7. 6名正常志愿者在另外两个日期接受研究,此前连续3天摄入每天提供30毫摩尔钠的饮食并在前一晚进行脱水。在这两天里,每名志愿者均接受背景静脉输注精氨酸加压素(5×10⁻⁷国际单位/千克·分钟),且一天接受静脉输注醋酸沙拉新(50纳克/千克·分钟)加载体,另一天仅接受载体。记录随后动脉压、尿溶质及无溶质水排泄的变化。8. 在输注沙拉新期间,收缩动脉压有小幅但显著的下降。(摘要截选至400词)

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本文引用的文献

1
Determination of inulin by means of resorcinol.用间苯二酚法测定菊粉。
Proc Soc Exp Biol Med. 1950 May;74(1):117-20. doi: 10.3181/00379727-74-17827.
5
Captopril kinetics.卡托普利动力学
Clin Pharmacol Ther. 1982 Apr;31(4):452-8. doi: 10.1038/clpt.1982.59.
9
Disposition of captopril in normal subjects.卡托普利在正常受试者体内的处置情况。
Clin Pharmacol Ther. 1980 May;27(5):636-41. doi: 10.1038/clpt.1980.90.
10

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