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Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice

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Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice. / Vitzthum, Helga; Seniuk, Anika; Schulte, Laura Helene; Müller, Maxie Luise; Hetz, Hannah; Ehmke, Heimo.

in: J PHYSIOL-LONDON, Jahrgang 592, Nr. Pt 5, 01.03.2014, S. 1139-57.

Publikationen: SCORING: Beitrag in Fachzeitschrift/ZeitungSCORING: ZeitschriftenaufsatzForschungBegutachtung

Harvard

Vitzthum, H, Seniuk, A, Schulte, LH, Müller, ML, Hetz, H & Ehmke, H 2014, 'Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice', J PHYSIOL-LONDON, Jg. 592, Nr. Pt 5, S. 1139-57. https://doi.org/10.1113/jphysiol.2013.266924

APA

Vitzthum, H., Seniuk, A., Schulte, L. H., Müller, M. L., Hetz, H., & Ehmke, H. (2014). Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice. J PHYSIOL-LONDON, 592(Pt 5), 1139-57. https://doi.org/10.1113/jphysiol.2013.266924

Vancouver

Vitzthum H, Seniuk A, Schulte LH, Müller ML, Hetz H, Ehmke H. Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice. J PHYSIOL-LONDON. 2014 Mär 1;592(Pt 5):1139-57. https://doi.org/10.1113/jphysiol.2013.266924

Bibtex

@article{e8c7a4215f0247ab8e17afd47c2d38f3,
title = "Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice",
abstract = "A network of kinases, including WNKs, SPAK and Sgk1, is critical for the independent regulation of K+ and Na+ transport in the distal nephron. Angiotensin II is thought to act as a key hormone in orchestrating these kinases to switch from K+ secretion during hyperkalaemia to Na+ reabsorption during intravascular volume depletion, thus keeping disturbances in electrolyte and blood pressure homeostasis at a minimum. It remains unclear, however, how K+ and Na+ transport are regulated during a high Na+ intake, which is associated with suppressed angiotensin II levels and a high distal tubular Na+ load. We therefore investigated the integrated blood pressure, renal, hormonal and gene and protein expression responses to large changes of K+ intake in Na+ replete mice. Both low and high K+ intake increased blood pressure and caused Na+ retention. Low K+ intake was accompanied by an upregulation of the sodium-chloride cotransporter (NCC) and its activating kinase SPAK, and inhibition of NCC normalized blood pressure. Renal responses were unaffected by angiotensin AT1 receptor antagonism, indicating that low K+ intake activates the distal nephron by an angiotensin-independent mode of action. High K+ intake was associated with elevated plasma aldosterone concentrations and an upregulation of the epithelial sodium channel (ENaC) and its activating kinase Sgk1. Surprisingly, high K+ intake increased blood pressure even during ENaC or mineralocorticoid receptor antagonism, suggesting the contribution of aldosterone-independent mechanisms. These findings show that in a Na+ replete state, changes in K+ intake induce specific molecular and functional adaptations in the distal nephron that cause a functional coupling of renal K+ and Na+ handling, resulting in Na+ retention and high blood pressure when K+ intake is either restricted or excessively increased.",
author = "Helga Vitzthum and Anika Seniuk and Schulte, {Laura Helene} and M{\"u}ller, {Maxie Luise} and Hannah Hetz and Heimo Ehmke",
year = "2014",
month = mar,
day = "1",
doi = "10.1113/jphysiol.2013.266924",
language = "English",
volume = "592",
pages = "1139--57",
journal = "J PHYSIOL-LONDON",
issn = "0022-3751",
publisher = "Wiley-Blackwell",
number = "Pt 5",

}

RIS

TY - JOUR

T1 - Functional coupling of renal K+ and Na+ handling causes high blood pressure in Na+ replete mice

AU - Vitzthum, Helga

AU - Seniuk, Anika

AU - Schulte, Laura Helene

AU - Müller, Maxie Luise

AU - Hetz, Hannah

AU - Ehmke, Heimo

PY - 2014/3/1

Y1 - 2014/3/1

N2 - A network of kinases, including WNKs, SPAK and Sgk1, is critical for the independent regulation of K+ and Na+ transport in the distal nephron. Angiotensin II is thought to act as a key hormone in orchestrating these kinases to switch from K+ secretion during hyperkalaemia to Na+ reabsorption during intravascular volume depletion, thus keeping disturbances in electrolyte and blood pressure homeostasis at a minimum. It remains unclear, however, how K+ and Na+ transport are regulated during a high Na+ intake, which is associated with suppressed angiotensin II levels and a high distal tubular Na+ load. We therefore investigated the integrated blood pressure, renal, hormonal and gene and protein expression responses to large changes of K+ intake in Na+ replete mice. Both low and high K+ intake increased blood pressure and caused Na+ retention. Low K+ intake was accompanied by an upregulation of the sodium-chloride cotransporter (NCC) and its activating kinase SPAK, and inhibition of NCC normalized blood pressure. Renal responses were unaffected by angiotensin AT1 receptor antagonism, indicating that low K+ intake activates the distal nephron by an angiotensin-independent mode of action. High K+ intake was associated with elevated plasma aldosterone concentrations and an upregulation of the epithelial sodium channel (ENaC) and its activating kinase Sgk1. Surprisingly, high K+ intake increased blood pressure even during ENaC or mineralocorticoid receptor antagonism, suggesting the contribution of aldosterone-independent mechanisms. These findings show that in a Na+ replete state, changes in K+ intake induce specific molecular and functional adaptations in the distal nephron that cause a functional coupling of renal K+ and Na+ handling, resulting in Na+ retention and high blood pressure when K+ intake is either restricted or excessively increased.

AB - A network of kinases, including WNKs, SPAK and Sgk1, is critical for the independent regulation of K+ and Na+ transport in the distal nephron. Angiotensin II is thought to act as a key hormone in orchestrating these kinases to switch from K+ secretion during hyperkalaemia to Na+ reabsorption during intravascular volume depletion, thus keeping disturbances in electrolyte and blood pressure homeostasis at a minimum. It remains unclear, however, how K+ and Na+ transport are regulated during a high Na+ intake, which is associated with suppressed angiotensin II levels and a high distal tubular Na+ load. We therefore investigated the integrated blood pressure, renal, hormonal and gene and protein expression responses to large changes of K+ intake in Na+ replete mice. Both low and high K+ intake increased blood pressure and caused Na+ retention. Low K+ intake was accompanied by an upregulation of the sodium-chloride cotransporter (NCC) and its activating kinase SPAK, and inhibition of NCC normalized blood pressure. Renal responses were unaffected by angiotensin AT1 receptor antagonism, indicating that low K+ intake activates the distal nephron by an angiotensin-independent mode of action. High K+ intake was associated with elevated plasma aldosterone concentrations and an upregulation of the epithelial sodium channel (ENaC) and its activating kinase Sgk1. Surprisingly, high K+ intake increased blood pressure even during ENaC or mineralocorticoid receptor antagonism, suggesting the contribution of aldosterone-independent mechanisms. These findings show that in a Na+ replete state, changes in K+ intake induce specific molecular and functional adaptations in the distal nephron that cause a functional coupling of renal K+ and Na+ handling, resulting in Na+ retention and high blood pressure when K+ intake is either restricted or excessively increased.

U2 - 10.1113/jphysiol.2013.266924

DO - 10.1113/jphysiol.2013.266924

M3 - SCORING: Journal article

C2 - 24396058

VL - 592

SP - 1139

EP - 1157

JO - J PHYSIOL-LONDON

JF - J PHYSIOL-LONDON

SN - 0022-3751

IS - Pt 5

ER -