Protein Phosphatase 1 Inhibitor–1 Mediates the cAMP-Dependent Stimulation of the Renal NaCl Cotransporter

Pentón, David; Moser, Sandra; Wengi, Agnieszka; Czogalla, Jan; Rosenbæk, Lena Lindtoft; Rigendinger, Fritz; Faresse, Nourdine; Martins, Joana Raquel; Fenton, Robert A.; Loffing‐Cueni, Dominique; Loffing, Johannes

doi:10.1681/asn.2018050540

Cited by 27 publications

(35 citation statements)

References 58 publications

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“…The role of PP1 was confirmed when the endogenous inhibitor of PP1, I-1, was deleted in mice, and pNCC levels decreased independent of total NCC abundance (242). Furthermore, PP1 interacts with NCC and can dephosphorylate it in vitro (239). The current view is that changes in cAMP, which can occur via, e.g., the ␤-adrenergic receptor or the vasopressin type 2 receptor (V2R), stimulates protein kinase A (PKA) to phosphorylate I-1, which inhibits PP1 and ultimately leads to an increase in pNCC.…”

Section: Regulation Of Ncc By Phosphatasesmentioning

confidence: 89%

Regulation of the Renal NaCl Cotransporter and Its Role in Potassium Homeostasis

Hoorn

Gritter

Cuevas³

et al. 2020

Physiological Reviews

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118

137

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Daily dietary potassium (K+) intake may be as large as the extracellular K+ pool. To avoid acute hyperkalemia, rapid removal of K+ from the extracellular space is essential. This is achieved by translocating K+ into cells and increasing urinary K+ excretion. Emerging data now indicate that the renal thiazide-sensitive NaCl cotransporter (NCC) is critically involved in this homeostatic kaliuretic response. This suggests that the early distal convoluted tubule (DCT) is a K+ sensor that can modify sodium (Na+) delivery to downstream segments to promote or limit K+ secretion. K+ sensing is mediated by the basolateral K+ channels Kir4.1/5.1, a capacity that the DCT likely shares with other nephron segments. Thus, next to K+-induced aldosterone secretion, K+ sensing by renal epithelial cells represents a second feedback mechanism to control K+ balance. NCC’s role in K+ homeostasis has both physiological and pathophysiological implications. During hypovolemia, NCC activation by the renin-angiotensin system stimulates Na+ reabsorption while preventing K+ secretion. Conversely, NCC inactivation by high dietary K+ intake maximizes kaliuresis and limits Na+ retention, despite high aldosterone levels. NCC activation by a low-K+ diet contributes to salt-sensitive hypertension. K+-induced natriuresis through NCC offers a novel explanation for the antihypertensive effects of a high-K+ diet. A possible role for K+ in chronic kidney disease is also emerging, as epidemiological data reveal associations between higher urinary K+ excretion and improved renal outcomes. This comprehensive review will embed these novel insights on NCC regulation into existing concepts of K+ homeostasis in health and disease.

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Section: Regulation Of Ncc By Phosphatasesmentioning

confidence: 89%

Regulation of the Renal NaCl Cotransporter and Its Role in Potassium Homeostasis

Hoorn

Gritter

Cuevas³

et al. 2020

Physiological Reviews

Self Cite

118

137

View full text Add to dashboard Cite

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“…Activation of α1-adrenoceptors inhibits the suppression of NCC during high salt intake via a WNK/SPAK/ OxSR1-dependent signaling pathway in rat kidneys (Frame et al, 2019). Dephosphorylation of NCC by the protein phosphatase 1 can be inhibited through a protein kinase A-dependent activation of the protein phosphatase 1 inhibitor via β1-adrenergic receptor activation (Penton et al, 2019).…”

Section: Effects Of Renal Sympathetic Norepinephrine Release and Epitmentioning

confidence: 99%

Role of α2-Adrenoceptors in Hypertension: Focus on Renal Sympathetic Neurotransmitter Release, Inflammation, and Sodium Homeostasis

et al. 2020

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“…In one of our earlier in vitro studies in Xenopus oocytes, NCC activity was found to be regulated by Protein phosphatase 4 (PP4) through its interaction with a conserved N‐terminal amino acid threonine 58 of NCC, and this regulation was independent of WNK4 regulated NCC trafficking to the membrane (Glover, Mercier Zuber, Figg, & O'Shaughnessy, ). More recently, signaling pathways independent of the WNK4/SPAK cascade have been shown to regulate NCC phosphorylation (and therefore its activity) in the DCT (Penton et al, ). In vitro studies showed that protein phosphatase 1 (PP1) dephosphorylates NCC whereas the PP1 inhibitor calyculin A had the opposite effect, and protein kinase A (PKA)‐dependent phosphorylation of the PP1 inhibitor 1 abolished the PP1‐mediated dephosphorylation of NCC in ex vivo mouse kidney preparations (Penton et al, ).…”

Section: Discussionmentioning

confidence: 99%

“…More recently, signaling pathways independent of the WNK4/SPAK cascade have been shown to regulate NCC phosphorylation (and therefore its activity) in the DCT (Penton et al, ). In vitro studies showed that protein phosphatase 1 (PP1) dephosphorylates NCC whereas the PP1 inhibitor calyculin A had the opposite effect, and protein kinase A (PKA)‐dependent phosphorylation of the PP1 inhibitor 1 abolished the PP1‐mediated dephosphorylation of NCC in ex vivo mouse kidney preparations (Penton et al, ). A comprehensive study of PP inhibitors in our cells has not been done to confirm if either PP1 or PP4 are important controllers of NCC dephosphorylation in our model HEK cells.…”

Section: Discussionmentioning

confidence: 99%

Modified HEK cells simulate DCT cells in their sensitivity and response to changes in extracellular K

Murthy

O’Shaughnessy

2019

Physiol Rep

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A potassium (K+) rich diet is known to have an antihypertensive effect that has been embodied by the NHLBI in the DASH diet. However, the molecular basis for this blood pressure‐lowering effect has been unclear, until a recent study proposed a model in which the DCT cells of the kidney regulate their salt transport in response to variations in intracellular chloride ([Cl−]i), which are directly regulated by serum K+. With the knowledge that WNK proteins are Cl− sensors, and are a part of the WNK/SPAK/NCC signaling cascade which regulates the NCC, the main salt transporter in the distal nephron, we examined the effect of serum K+ on the ([Cl−]i) and, in turn its effect on the WNK4 signaling pathway in a “modified HEK 293T” cell line. Using a fluorescence‐based approach in this cell line, we have shown that the membrane potential of the cell membrane is sensitive to the small changes in external KCl within the physiological range (2–5 mM), thus functioning as a K+ electrode. When the extracellular K+ was progressively increased (2–5 mM), the membrane depolarization lead to a subsequent increase in [Cl−]i measured by fluorescence quenching of an intracellular chloride sensor. Increase in extracellular [K] resulted in a decrease in the phosphorylation of the WNK4 protein and its downstream targets, SPAK and NCC. This confirms that small changes in serum K can affect WNK4/SPAK/NCC signaling and transcellular Na+ flux through the DCT and provide a possible mechanism by which a K‐rich DASH diet could reduce blood pressure.

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Protein Phosphatase 1 Inhibitor–1 Mediates the cAMP-Dependent Stimulation of the Renal NaCl Cotransporter

Cited by 27 publications

References 58 publications

Regulation of the Renal NaCl Cotransporter and Its Role in Potassium Homeostasis

Regulation of the Renal NaCl Cotransporter and Its Role in Potassium Homeostasis

Role of α2-Adrenoceptors in Hypertension: Focus on Renal Sympathetic Neurotransmitter Release, Inflammation, and Sodium Homeostasis

Modified HEK cells simulate DCT cells in their sensitivity and response to changes in extracellular K

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