mTORC2 critically regulates renal potassium handling
Florian Grahammer, Viatcheslav Nesterov, Azaz Ahmed, Frederic Steinhardt, Lukas Sandner, Frederic Arnold, Tomke Cordts, Silvio Negrea, Marko Bertog, Marcus A. Ruegg, Michael N. Hall, Gerd Walz, Christoph Korbmacher, Ferruh Artunc, Tobias B. Huber
Florian Grahammer, Viatcheslav Nesterov, Azaz Ahmed, Frederic Steinhardt, Lukas Sandner, Frederic Arnold, Tomke Cordts, Silvio Negrea, Marko Bertog, Marcus A. Ruegg, Michael N. Hall, Gerd Walz, Christoph Korbmacher, Ferruh Artunc, Tobias B. Huber
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Research Article Nephrology

mTORC2 critically regulates renal potassium handling

Abstract

The mTOR pathway orchestrates cellular homeostasis. The rapamycin-sensitive mTOR complex (mTORC1) in the kidney has been widely studied; however, mTORC2 function in renal tubules is poorly characterized. Here, we generated mice lacking mTORC2 in the distal tubule (Rictorfl/fl Ksp-Cre mice), which were viable and had no obvious phenotype, except for a 2.5-fold increase in plasma aldosterone. Challenged with a low-Na+ diet, these mice adequately reduced Na+ excretion; however, Rictorfl/fl Ksp-Cre mice rapidly developed hyperkalemia on a high-K+ diet, despite a 10-fold increase in serum aldosterone levels, implying that mTORC2 regulates kaliuresis. Phosphorylation of serum- and glucocorticoid-inducible kinase 1 (SGK1) and PKC-α was absent in Rictorfl/fl Ksp-Cre mice, indicating a functional block in K+ secretion activation via ROMK channels. Indeed, patch-clamp experiments on split-open tubular segments from the transition zone of the late connecting tubule and early cortical collecting duct demonstrated that Ba2+-sensitive apical K+ currents were barely detectable in the majority of Rictorfl/fl Ksp-Cre mice. Conversely, epithelial sodium channel (ENaC) activity was largely preserved, suggesting that the reduced ability to maintain K+ homeostasis is the result of impaired apical K+ conductance and not a reduced electrical driving force for K+ secretion. Thus, these data unravel a vital and nonredundant role of mTORC2 for distal tubular K+ handling.

Authors

Florian Grahammer, Viatcheslav Nesterov, Azaz Ahmed, Frederic Steinhardt, Lukas Sandner, Frederic Arnold, Tomke Cordts, Silvio Negrea, Marko Bertog, Marcus A. Ruegg, Michael N. Hall, Gerd Walz, Christoph Korbmacher, Ferruh Artunc, Tobias B. Huber

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Figure 2

Distal tubular mTORC2 deletion is a key survival factor in response to electrolyte challenges.

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Distal tubular mTORC2 deletion is a key survival factor in response to e...
(A) After 4 days on the indicated diets, Rictorfl/fl Ksp-Cre mice only lost weight under low-Na+/high-K+ (LS/HK) and normal Na+/HK (NS/HK) diets but not under LS/normal K+ (LS/NK) or high-Na+/HK (HS/HK) diets. (B) Despite striking elevations of plasma aldosterone, (C) Rictorfl/fl Ksp-Cre animals, in contrast to control mice, developed hyperkalemia under a HK diet that got more severe as the Na+ content was lowered. (D) Virtually all diuretics either directly or indirectly act on the ASDN. We tested the response to oral furosemide (Furo), hydrochlorothiazide (HCT), and triamterene (Triam) for 5 days. Similar to HK diet, Rictorfl/fl Ksp-Cre mice lost 20% of their body weight under triamterene, while weight loss was modest for furosemide and HCT. (E) Similar to LS/HK diet, triamterene led to hyperkalemia, (F) again despite maximal secretion of aldosterone, which reached higher levels with the more distal block of the diuretic (ANOVA; #P < 0.05; ##P < 0.01; ###P < 0.001; n = 4–30).