Essential role of Kir5.1 channels in renal salt handling and blood pressure control
Oleg Palygin, Vladislav Levchenko, Daria V. Ilatovskaya, Tengis S. Pavlov, Oleh M. Pochynyuk, Howard J. Jacob, Aron M. Geurts, Matthew R. Hodges, Alexander Staruschenko
Oleg Palygin, Vladislav Levchenko, Daria V. Ilatovskaya, Tengis S. Pavlov, Oleh M. Pochynyuk, Howard J. Jacob, Aron M. Geurts, Matthew R. Hodges, Alexander Staruschenko
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Research Article Nephrology

Essential role of Kir5.1 channels in renal salt handling and blood pressure control

Abstract

Supplementing diets with high potassium helps reduce hypertension in humans. Inwardly rectifying K+ channels Kir4.1 (Kcnj10) and Kir5.1 (Kcnj16) are highly expressed in the basolateral membrane of distal renal tubules and contribute to Na+ reabsorption and K+ secretion through the direct control of transepithelial voltage. To define the importance of Kir5.1 in blood pressure control under conditions of salt-induced hypertension, we generated a Kcnj16 knockout in Dahl salt-sensitive (SS) rats (SSKcnj16–/–). SSKcnj16–/– rats exhibited hypokalemia and reduced blood pressure, and when fed a high-salt diet (4% NaCl), experienced 100% mortality within a few days triggered by salt wasting and severe hypokalemia. Electrophysiological recordings of basolateral K+ channels in the collecting ducts isolated from SSKcnj16–/– rats revealed activity of only homomeric Kir4.1 channels. Kir4.1 expression was upregulated in SSKcnj16–/– rats, but the protein was predominantly localized in the cytosol in SSKcnj16–/– rats. Benzamil, but not hydrochlorothiazide or furosemide, rescued this phenotype from mortality on a high-salt diet. Supplementation of high-salt diet with increased potassium (2% KCl) prevented mortality in SSKcnj16–/– rats and prevented or mitigated hypertension in SSKcnj16–/– or control SS rats, respectively. Our results demonstrate that Kir5.1 channels are key regulators of renal salt handling in SS hypertension.

Authors

Oleg Palygin, Vladislav Levchenko, Daria V. Ilatovskaya, Tengis S. Pavlov, Oleh M. Pochynyuk, Howard J. Jacob, Aron M. Geurts, Matthew R. Hodges, Alexander Staruschenko

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Figure 8

Changes in ENaC, NCC, and NKCC2 expression in SS and SSKcnj16–/– rats fed a high-potassium diet.

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Changes in ENaC, NCC, and NKCC2 expression in SS and SSKcnj16–/– rats fe...
Western blotting analysis of NCC, p-NCC, NKCC2, and p-NKCC (A) and α-, β-, and γ-ENaC subunits (truncated forms of α- and γ-ENaC subunits are also shown) (B) from the kidney cortex lysates of salt-sensitive (SS) rats were fed either a standard 4% NaCl diet or a 4% NaCl diet supplemented with high K+ (2% KCl) and SSKcnj16–/– rats fed a 4% NaCl diet supplemented with high K+. Each line represents 1 rat. (C) Summary graphs represent the average relative density of the bands (normalized to loading controls) in the groups. Comparisons between groups were made using 1-way ANOVA. *P < 0.05.