AJP - Renal Physiology, Vol 265, Issue 3 385-F390, Copyright © 1993 by American Physiological Society
The urease inhibitor acetohydroxamic acid is transported by the urea pathway in rat terminal IMCD
R. A. Star, A. D. Gillin, V. J. Parikh and J. M. Sands
Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas 75235-8856.
Acetohydroxamic acid (AHA), a urea analogue, is used clinically to dissolve
struvite stones because it inhibits the urease produced by Proteus
mirabilis. To be effective, the concentration of AHA must be high in the
collecting duct system and final urine. Because AHA is structurally similar
to urea, we investigated whether AHA is transported by the urea carrier
found in the terminal inner medullary collecting duct (IMCD) and the
erythrocyte. We examined AHA transport under four conditions known to
affect urea movement across the terminal IMCD, i.e., stimulation by
vasopressin (AVP) and hyperosmolality, and inhibition by phloretin and urea
analogues. The AHA permeability was determined with a 10 mM bath-to-lumen
AHA gradient. AHA was measured by ultramicrocolorimetry. Addition of 1 nM
AVP to the bath increased the AHA permeability of the perfused terminal
IMCD. Increasing perfusate and bath osmolality from 290 to 690 mosmol/kgH2O
(by adding NaCl) also increased tubule permeability to AHA. Addition of
either 0.25 mM phloretin to the bath or 200 mM thiourea to the lumen
reversibly inhibited the AVP-stimulated AHA permeability. AHA-induced
osmotic lysis of erythrocytes was inhibited by phloretin or
thionicotinamide; AHA inhibited the osmotic lysis induced by the urea
analogue acetamide. Thus, in the rat terminal IMCD, both urea and AHA
transport are stimulated by AVP and hyperosmolality, and both are inhibited
by phloretin and thiourea. In erythrocytes, both urea and AHA transport are
inhibited by phloretin or thionicotinamide. Thus AHA is transported by the
urea carrier in the terminal IMCD and erythrocyte.(ABSTRACT TRUNCATED AT
250 WORDS)
