Renal Deletion of 12 kDa FK506-Binding Protein Attenuates Tacrolimus-Induced Hypertension

Lazelle, Rebecca; McCully, Belinda H.; Terker, Andrew S.; Himmerkus, Nina; Blankenstein, Katharina I.; Mutig, Kerim; Bleich, Markus; Bachmann, S.; Yang, Chao; Ellison, David H.

doi:10.1681/asn.2015040466

Cited by 48 publications

(51 citation statements)

References 25 publications

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“…Similarly, a kidney‐specific deletion of FK506 binding protein, crucial for the effects of tacrolimus on PP3, attenuates tacrolimus‐induced arterial hypertension (Lazelle et al . ). However, in our experiments, inhibition of PP1 and PP3 did not block the [K + ] ex ‐induced dephosphorylation of NCC, suggesting that other signalling cascades are involved.…”

Section: Discussionmentioning

confidence: 97%

Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms

Pentón

Czogalla

Wengi

et al. 2016

The Journal of Physiology

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117

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A high dietary potassium (K + ) intake causes a rapid dephosphorylation, and hence inactivation, of the thiazide-sensitive NaCl cotransporter (NCC) in the renal distal convoluted tubule (DCT). Based on experiments in heterologous expression systems, it was proposed that changes in extracellular K+ concentration ([K + ]ex ) modulate NCC phosphorylation via a Cl − -dependent modulation of the with no lysine (K) kinases (WNK)-STE20/SPS-1-44 related proline-alanine-rich protein kinase (SPAK)/oxidative stress-related kinase (OSR1) kinase pathway. We used the isolated perfused mouse kidney technique and ex vivo preparations of mouse kidney slices to test the physiological relevance of this model on native DCT Key points summary:• High dietary potassium (K + ) intake dephosphorylates and inactivates the NaCl cotransporter (NCC) in the renal distal convoluted tubule (DCT).• Using several ex-vivo models, we show that physiological changes in extracellular K + , like those occurring after a K + rich diet, are sufficient to promote a very rapid dephosphorylation of NCC in native DCT cells.• Whilst the increase of NCC phosphorylation upon decreased extracellular K + appears to depend on cellular Cl -fluxes, the rapid NCC dephosphorylation in response to increased extracellular K + is not Cl -dependent.• The Cl -dependent pathway involves the SPAK/OSR1 kinases, whereas the Cl -independent pathway may include additional signaling cascades.

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Section: Discussionmentioning

confidence: 97%

Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms

Pentón

Czogalla

Wengi

et al. 2016

The Journal of Physiology

Self Cite

117

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“…In a study using a kidney specific 12 kDa FK506-binding protein, FKBP12, knockout mice, Tac caused hypertension by inhibiting calcineurin directly in DCT cells expressing NCC [22]. Moreover, NCC knockout mice were protected from tacrolimus-induced hypertension [21], confirming the role of NCC in CNI-induced hypertension.…”

Section: Discussionmentioning

confidence: 98%

NaCl cotransporter abundance in urinary vesicles is increased by calcineurin inhibitors and predicts thiazide sensitivity

et al. 2017

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Animal studies have shown that the calcineurin inhibitors (CNIs) cyclosporine and tacrolimus can activate the thiazide-sensitive NaCl cotransporter (NCC). A common side effect of CNIs is hypertension. Renal salt transporters such as NCC are excreted in urinary extracellular vesicles (uEVs) after internalization into multivesicular bodies. Human studies indicate that CNIs also increase NCC abundance in uEVs, but results are conflicting and no relationship with NCC function has been shown. Therefore, we investigated the effects of CsA and Tac on the abundance of both total NCC (tNCC) and phosphorylated NCC at Thr60 phosphorylation site (pNCC) in uEVs, and assessed whether NCC abundance in uEVs predicts the blood pressure response to thiazide diuretics. Our results show that in kidney transplant recipients treated with cyclosporine (n = 9) or tacrolimus (n = 23), the abundance of both tNCC and pNCC in uEVs is 4–5 fold higher than in CNI-free kidney transplant recipients (n = 13) or healthy volunteers (n = 6). In hypertensive kidney transplant recipients, higher abundances of tNCC and pNCC prior to treatment with thiazides predicted the blood pressure response to thiazides. During thiazide treatment, the abundance of pNCC in uEVs increased in responders (n = 10), but markedly decreased in non-responders (n = 8). Thus, our results show that CNIs increase the abundance of both tNCC and pNCC in uEVs, and these increases correlate with the blood pressure response to thiazides. This implies that assessment of NCC in uEVs could represent an alternate method to guide anti-hypertensive therapy in kidney transplant recipients.

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“…First, although the Pax8 system is relatively specific for kidney epithelia, 34,35 substantial gene deletion also occurs in the liver, which may have contributed to extrarenal K + uptake. Second, extrarenal MR may be stimulated in KS MR 2/2 mice at baseline, because plasma [aldosterone] is elevated; the addition of supraphysiologic aldosterone, then, may have little additional effect.…”

Section: Discussionmentioning

confidence: 99%

Direct and Indirect Mineralocorticoid Effects Determine Distal Salt Transport

Terker

Yarbrough

Ferdaus

et al. 2015

JASN

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113

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Excess aldosterone is an important contributor to hypertension and cardiovascular disease. Conversely, low circulating aldosterone causes salt wasting and hypotension. Aldosterone activates mineralocorticoid receptors (MRs) to increase epithelial sodium channel (ENaC) activity. However, aldosterone may also stimulate the thiazide-sensitive Na + -Cl 2 cotransporter (NCC). Here, we generated mice in which MRs could be deleted along the nephron to test this hypothesis. These kidney-specific MR-knockout mice exhibited salt wasting, low BP, and hyperkalemia. Notably, we found evidence of deficient apical orientation and cleavage of ENaC, despite the salt wasting. Although these mice also exhibited deficient NCC activity, NCC could be stimulated by restricting dietary potassium, which also returned BP to control levels. Together, these results indicate that MRs regulate ENaC directly, but modulation of NCC is mediated by secondary changes in plasma potassium concentration. Electrolyte balance and BP seem to be determined, therefore, by a delicate interplay between direct and indirect mineralocorticoid actions in the distal nephron.

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Renal Deletion of 12 kDa FK506-Binding Protein Attenuates Tacrolimus-Induced Hypertension

Cited by 48 publications

References 25 publications

Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms

Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms

NaCl cotransporter abundance in urinary vesicles is increased by calcineurin inhibitors and predicts thiazide sensitivity

Direct and Indirect Mineralocorticoid Effects Determine Distal Salt Transport

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Renal Deletion of 12 kDa FK506-Binding Protein Attenuates Tacrolimus-Induced Hypertension

Cited by 48 publications

References 25 publications

Extracellular K+ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl−‐dependent and independent mechanisms

Extracellular K+ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl−‐dependent and independent mechanisms

NaCl cotransporter abundance in urinary vesicles is increased by calcineurin inhibitors and predicts thiazide sensitivity

Direct and Indirect Mineralocorticoid Effects Determine Distal Salt Transport

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Resources

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Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms

Extracellular K⁺ rapidly controls NaCl cotransporter phosphorylation in the native distal convoluted tubule by Cl⁻‐dependent and independent mechanisms