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氨氯吡咪对原发性醛固酮增多症和巴特综合征中肾素-醛固酮系统的影响。

The effect of amiloride on the renin-aldosterone system in primary hyperaldosteronism and Bartter's syndrome.

作者信息

Griffing G T, Aurecchia S A, Sindler B H, Melby J C

出版信息

J Clin Pharmacol. 1982 Nov-Dec;22(11-12):505-12. doi: 10.1002/j.1552-4604.1982.tb02643.x.

Abstract

Amiloride is a potassium-sparing diuretic which has been advocated for the treatment of hypokalemic disorders. This agent was prospectively evaluated in hypokalemic patients with either primary hyperaldosteronism (ten patients) or Bartter's syndrome (five patients). Vital signs, electrolytes, and ambulatory hormonal studies were assessed during a control period and treatment period with amiloride therapy at 10 to 40 mg/day over two to 24 weeks. During the treatment period the systolic and diastolic blood pressure fell significantly in primary hyperaldosteronism but remained unchanged in Bartter's syndrome. In summary, amiloride therapy (1) increased plasma potassium in both diseases; (2) increased plasma renin activity (PRA) in primary hyperaldosteronism but decreased PRA in Bartter's syndrome; and (3) increased plasma aldosterone in both diseases. Since potassium is known to suppress renin production and stimulate aldosterone secretion, correction of the hypokalemia in this study probably accounts for the decreased PRA and increased plasma aldosterone observed in Bartter's syndrome. The increase in both PRA and plasma aldosterone in primary hyperaldosteronism, however, may be evidence of either a direct activation of the renin-aldosterone system or, alternatively, may be due to the mild natriuretic effects of amiloride.

摘要

氨氯吡咪是一种保钾利尿剂,已被推荐用于治疗低钾血症。对10例原发性醛固酮增多症患者和5例巴特综合征患者进行前瞻性评估。在对照期和治疗期,采用氨氯吡咪治疗,剂量为10至40毫克/天,持续2至24周,期间评估生命体征、电解质和动态激素水平。在治疗期,原发性醛固酮增多症患者的收缩压和舒张压显著下降,而巴特综合征患者的血压保持不变。总之,氨氯吡咪治疗(1)在两种疾病中均提高了血钾水平;(2)在原发性醛固酮增多症中提高了血浆肾素活性(PRA),但在巴特综合征中降低了PRA;(3)在两种疾病中均提高了血浆醛固酮水平。由于已知钾可抑制肾素生成并刺激醛固酮分泌,本研究中低钾血症的纠正可能是巴特综合征中PRA降低和血浆醛固酮升高的原因。然而,原发性醛固酮增多症中PRA和血浆醛固酮的升高,可能是肾素-醛固酮系统直接激活的证据,或者也可能是由于氨氯吡咪的轻度利钠作用。

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