Publication
Activation of the Hypoxia-Inducible Factor Pathway Inhibits Epithelial Sodium Channel–Mediated Sodium Transport in Collecting Duct Principal Cells
Publisher:
Ovid Technologies (Wolters Kluwer Health)
Date:
12-2021
DOI:
10.1681/ASN.2021010046
Abstract: The hypoxia-inducible factor (HIF) pathway is a key mediator of cellular adaptation to low oxygen tension. The aldosterone-sensitive distal nephron is the site of active and highly ATP-consuming sodium reabsorption, according to the requirement of sodium balance. The authors found that activation of the HIF pathway in cultured principal cells led to decreased amiloride-sensitive current (reflecting decreased epithelial sodium channel [ENaC] activity) and decreased expression of ENaC subunits, whereas HIF silencing led to increased amiloride-sensitive current and expression of ENaC subunits. Hypoxic control mice displayed decreased γ ENaC, whereas HIF1 α knockout mice displayed increased γ ENaC. These findings suggest that the HIF pathway controls ENaC expression and activity, and may represent a negative feedback mechanism to prevent hypoxia and/or reactive oxygen species–induced cell damage under sustained stimulation of sodium transport. Active sodium reabsorption is the major factor influencing renal oxygen consumption and production of reactive oxygen species (ROS). Increased sodium reabsorption uses more oxygen, which may worsen medullary hypoxia and produce more ROS via enhanced mitochondrial ATP synthesis. Both mechanisms may activate the hypoxia-inducible factor (HIF) pathway. Because the collecting duct is exposed to low oxygen pressure and variations of active sodium transport, we assessed whether the HIF pathway controls epithelial sodium channel (ENaC)–dependent sodium transport. We investigated HIF’s effect on ENaC expression in mpkCCD cl4 cells (a model of collecting duct principal cells) using real-time PCR and western blot and ENaC activity by measuring amiloride-sensitive current. We also assessed the effect of hypoxia and sodium intake on abundance of kidney sodium transporters in wild-type and inducible kidney tubule–specific Hif1α knockout mice. In cultured cells, activation of the HIF pathway by dimethyloxalylglycine or hypoxia inhibited sodium transport and decreased expression of β ENaC and γ ENaC, as well as of Na,K-ATPase. HIF1 α silencing increased β ENaC and γ ENaC expression and stimulated sodium transport. A constitutively active mutant of HIF1 α produced the opposite effect. Aldosterone and inhibition of the mitochondrial respiratory chain slowly activated the HIF pathway, suggesting that ROS may also activate HIF. Decreased γ ENaC abundance induced by hypoxia in normal mice was abolished in Hif1α knockout mice. Similarly, Hif1α knockout led to increased γ ENaC abundance under high sodium intake. This study reveals that γ ENaC expression and activity are physiologically controlled by the HIF pathway, which may represent a negative feedback mechanism to preserve oxygenation and/or prevent excessive ROS generation under increased sodium transport.