In vivo stimulation of apical P2 receptors in collecting ducts: evidence for inhibition of sodium reabsorption
- 1 June 2005
- journal article
- Published by American Physiological Society in American Journal of Physiology-Renal Physiology
- Vol. 288 (6) , F1243-F1248
- https://doi.org/10.1152/ajprenal.00152.2004
Abstract
In vitro evidence suggests that intraluminal nucleotides, acting on apical P2 receptors, may influence amiloride-sensitive sodium reabsorption in collecting ducts. The present study has assessed this possibility directly in anesthetized rats, by determining the urinary recovery of22Na relative to that of [14C]inulin (Na/inulin recovery ratio) during in vivo microperfusion of late distal tubules with artificial tubular fluid containing various P2 agonists (all at 1 mM). In animals maintained on a control diet, in which amiloride-sensitive22Na reabsorption was modest, the poorly hydrolysable, broad-spectrum P2 agonist ATPγS had no significant effect on the Na/inulin recovery ratio. In contrast, in rats maintained on a low-sodium diet, in which amiloride-sensitive22Na reabsorption was considerably enhanced, ATPγS caused a significant increase in the Na/inulin recovery ratio (control: 14 ± 3%; ATPγS: 28 ± 4%; n = 32 pairs; P < 0.001, paired t-test). No change in the Na/inulin recovery ratio was seen in time controls (13 ± 3 vs. 14 ± 4%; n = 15 pairs). In subsequent experiments in rats maintained on a low-sodium diet, we used more selective agonists in an attempt to identify the receptor subtype responsible for the effect of ATPγS. The P2Y1agonist 2meSADP, the P2Y2/4agonists Ap4A and Cp4U, and the P2X agonist BzATP were all without significant effect on the Na/inulin recovery ratio. These findings constitute the first in vivo evidence for a functional role for apical P2 receptors in collecting ducts, but the identity of the receptor subtype(s) involved remains elusive.Keywords
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