Urinary Kallikrein Excretion in Normal Man: Relationships to Sodium Intake and Sodium-Retaining Steroids

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Circulation Research. 1974;35:812-819

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(Circulation Research. 1974;35:812.)
© 1974 American Heart Association, Inc.

Urinary Kallikrein Excretion in Normal Man

Relationships to Sodium Intake and Sodium-Retaining Steroids

HARRY S. MARGOLIUS ¹, DAVID HORWITZ ¹, RONALD G. GELLER ¹, R. WAYNE Alexander ¹, JOHN R. GILL. Jr. ¹, JOHN J. PISANO ¹, HARRY R. KEISER ¹

¹ Hypertension-Endocrine Branch, National Heart and Lung Institute, National Institutes of Health Bethesda, Maryland 20014

The urinary excretion of kallikrein, a renal enzyme that cleavesthe potent vasodilator kinin, kallidin, from kininogen, wasmeasured in normal volunteers by three different assays, oneof which was a bioassay. When sodium intake was changed fromad libitum or 109 mEq/day to 9 mEq/day, daily kallikrein excretionincreased progressively in every subject to a mean maximal valuethat was 271% of control by day 7; an increase in sodium intaketo 259 mEq/day resulted in the return of kallikrein excretionto control values. Urinary excretion of amylase, a protein witha molecular weight similar to that of kallikrein, did not changewhen sodium intake was changed, but plasma renin activity andaldosterone excretion changed appropriately. In subjects ona constant-sodium (109 mEq/day), constant-potassium (100 mEq/day)diet, fludrocortisone, 0.5 mg/day for 10 days, increased kallikreinexcretion to a mean maximal value that was 203% of control.In subjects on a diet containing 9 mEq sodium/day, elevatedkallikrein excretion decreased during treatment with spironolactone,400 mg/day. Rapid administration of water (1 or 2 liters in30 minutes, orally) or rapid infusion of 2.4 liters of normalsaline did not significantly alter urinary kallikrein excretiondespite large changes in urine volume or sodium excretion. Thus,kallikrein excretion appears to be directly related to the effectivelevel of circulating sodium-retaining steroid. The findingsare consistent with a role for the kallikrein-kinin system inthe renal response to sodium-retaining hormones.

Key Words: low dietary sodium • high dietary sodium • spironolactone • renin • aldosterone • fludrocortisone

Accepted on August 11, 1974

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