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Research Article Free access | 10.1172/JCI106668

The effect of ketone bodies on renal ammoniogenesis

Guy Lemieux, Patrick Vinay, Pierre Robitaille, Gérard E. Plante, Yolande Lussier, and Pierre Martin

Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Renal Laboratory, Hôtel-Dieu Hospital and the Department of Medicine, University of Montreal School of Medicine, Montreal, Quebec, Canada

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Published September 1, 1971 - More info

Published in Volume 50, Issue 9 on September 1, 1971
J Clin Invest. 1971;50(9):1781–1791. https://doi.org/10.1172/JCI106668.
© 1971 The American Society for Clinical Investigation
Published September 1, 1971 - Version history
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Abstract

Infusion of ketone bodies to ammonium chloride-loaded acidotic dogs was found to induce significant reduction in urinary excretion of ammonia. This effect could not be attributed to urinary pH variations. Total ammonia production by the left kidney was measured in 25 animals infused during 90 min with the sodium salt of D,L-β-hydroxybutyric acid adjusted to pH 6.0 or 4.2. Ketonemia averaged 4.5 mM/liter. In all experiments the ammonia content of both urine and renal venous blood fell markedly so that ammoniogenesis was depressed by 60% or more within 60 min after the onset of infusion. Administration of equimolar quantities of sodium acetoacetate adjusted to pH 6.0 resulted in a 50% decrease in renal ammonia production. Infusion of ketone bodies adjusted to pH 6.0 is usually accompanied by a small increase in extracellular bicarbonate (3.7 mM/liter). However infusion of D,L-sodium lactate or sodium bicarbonate in amounts sufficient to induce a similar rise in plasma bicarbonate resulted in only a slight decrement in ammonia production (15%). The continuous infusion of 5% mannitol alone during 90-150 min failed to influence renal ammoniogenesis. Infusion of pure sodium-free β-hydroxybutyric acid prepared by ion exchange (pH 2.2) resulted in a 50% decrease in renal ammoniogenesis in spite of the fact that both urinary pH and plasma bicarbonate fell significantly. During all experiments where ketones were infused, the renal extraction of glutamine became negligible as the renal glutamine arteriovenous difference was abolished. Renal hemodynamics did not vary significantly. Infusion of β-hydroxybutyrate into the left renal artery resulted in a rapid decrease in ammoniogenesis by the perfused kidney. The present study indicates that ketone bodies exert their inhibitory influence within the renal tubular cell. Since their effect is independent of urinary or systemic acid-base changes, it is suggested that they depress renal ammoniogenesis by preventing the transformation of glutamine and glutamate into α-ketoglutarate in the mitochondria of the renal tubular cell.

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