4.5 Article

Evidence that renal arterial-venous oxygen shunting contributes to dynamic regulation of renal oxygenation

Journal

AMERICAN JOURNAL OF PHYSIOLOGY-RENAL PHYSIOLOGY
Volume 292, Issue 6, Pages F1726-F1733

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajprenal.00436.2006

Keywords

arteriovenous shunt; diffusional shunt; hypoxia; ischemia

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Renal blood flow (RBF) can be reduced in rats and rabbits by up to 40% without significant changes in renal tissue P-O2. We determined whether this occurs because renal oxygen consumption changes with RBF or due to some other mechanism. The relationships between RBF and renal cortical and medullary tissue P-O2 and renal oxygen metabolism were determined in the denervated kidneys of anesthetized rabbits under hypoxic, normoxic, and hyperoxic conditions. During artificial ventilation with 21% oxygen ( normoxia), RBF increased 32 +/- 8% during renal arterial infusion of acetylcholine and reduced 31 +/- 5% during ANG II infusion. Neither infusion significantly altered arterial pressure, tissue PO2 in the renal cortex or medulla, nor renal oxygen consumption. However, fractional oxygen extraction fell as RBF increased and the ratio of oxygen consumption to sodium reabsorption increased during ANG II infusion. Ventilation with 10% oxygen (hypoxia) significantly reduced both cortical and medullary P-O2 (60-70%), whereas ventilation with 50% and 100% oxygen (hyperoxia) increased cortical and medullary P-O2 (by 62-298 and 30-56%, respectively). However, responses to altered RBF under hypoxic and hyperoxic conditions were similar to those under normoxic conditions. Thus renal tissue PO2 was relatively independent of RBF within a physiological range (+/- 30%). This was not due to RBF-dependent changes in renal oxygen consumption. The observation that fractional extraction of oxygen fell with increased RBF, yet renal parenchymal PO2 remained unchanged, supports the hypothesis that preglomerular diffusional shunting of oxygen from arteries to veins increases with increasing RBF, and so contributes to dynamic regulation of intrarenal oxygenation.

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