Aldosterone stimulates vacuolar H<sup>+</sup>-ATPase activity in renal acid-secretory intercalated cells mainly via a protein kinase C-dependent pathway

Winter, Christian; Kampik, Nicole B.; Vedovelli, Luca; Rothenberger, Florina; Păunescu, Teodor G.; Stehberger, Paul A.; Brown, Dennis; John, Hubert; Wagner, Carsten A.

doi:10.1152/ajpcell.00076.2011

Cited by 46 publications

(41 citation statements)

References 71 publications

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“…Both our in vivo and in vitro data demonstrate that effectors of the PKA (cpt-cAMP) and PKC (DOG) pathways mimic the effect of aldosterone on caput clear cell activity. These results are in agreement with our previous studies showing activation of V-ATPase-dependent proton secretion in renal intercalated cells by these agonists (63). Previous results from our group have also shown that luminal delivery of drugs that stimulate either the PKA or PKC pathways increase clear cell activity (6,40).…”

Section: Discussionsupporting

confidence: 93%

“…These results indicate an amplification of the amount of V-ATPase present at the cell surface via either activation of the exocytosis of V-ATPase-rich vesicles or via inhibition of endocytosis. As a positive control we also analyzed sections from the kidney of mice treated with aldosterone, cpt-cAMP, or DOG and observed increased V-ATPase-rich microvilli projections in intercalated cells (data not shown), similar to our recently published observations (43,63). In addition to being regulated via recycling mechanisms, previous studies conducted mainly in yeast and insects have shown that V-ATPase activity can also be regulated via local assembly/disassembly of V-ATPase subunits (12,30,57).…”

Section: Discussionsupporting

confidence: 84%

“…Previous results from our group have also shown that luminal delivery of drugs that stimulate either the PKA or PKC pathways increase clear cell activity (6,40). In the kidney it was suggested that the PKC pathway contributes more than the PKA pathway to the nongenomic effect of aldosterone on intercalated cell V-ATPase activity (63). In the epididymis we show here that the effect of aldosterone is PKC but not PKA dependent because chelerythrine, but not mPKI inhibited the stimulatory effect of aldosterone on V-ATPase activity.…”

Section: Discussionmentioning

confidence: 79%

“…A 200-l bolus of either PBS, aldosterone (200 nM, Sigma-Aldrich), 8-(4-chlorophenylthio)adenosine 3=,5=-cylic monophosphate (cpt-cAMP; 20 mM, Sigma-Aldrich), or 1,2-dioctanoyl-sn-glycerol (DOG; 20 M, Sigma-Aldrich) was first injected and was then followed by an infusion of 600 l of either PBS or drug over 15 min using an infusion pump (KdScientific, Holliston, MA) at a rate of 2.4 ml/h. The doses used here are based on previously published studies showing activation of V-ATPase-proton secretion in renal intercalated cells by these agonists in vivo (43,63,64). The final aldosterone concentration injected into the animals was estimated to be ϳ1.55 nM, based on an average extracellular fluid volume of 103 ml for an adult rat (21,33,36,60).…”

Section: Methodsmentioning

confidence: 99%

“…Traditionally the cellular responses to aldosterone have been associated with genomic effects. However, recent studies have also shown a direct nongenomic regulation of intercalated cell function in the kidney by aldosterone (63,64). Intercalated cells are similar to epididymal clear cells; they can also express high levels of V-ATPase in their plasma membrane and are involved in luminal acidification in the kidney.…”

mentioning

confidence: 99%

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Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Roy

Hill

Ruan

et al. 2013

American Journal of Physiology-Cell Physiology

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ϩ -ATPase (V-ATPase) and acidify the lumen of the epididymis, a process that is essential for male fertility. The renin-angiotensin-aldosterone system (RAAS) regulates fluid and electrolyte balance in the epididymis, and a previous study showed binding of aldosterone exclusively to epididymal clear cells (Hinton BT, Keefer DA. Steroid Biochem 23: 231-233, 1985). We examined here the role of aldosterone in the regulation of V-ATPase in the epididymis. RT-PCR showed expression of the mineralocorticoid receptor [MR; nuclear receptor subfamily 3, group C member 2 (NR3C2)] and 11-␤-dehydrogenase isozyme 2 (HSD11␤2) mRNAs specifically in clear cells, isolated by fluorescence-activated cell sorting from B1-enhanced green fluorescent protein (EGFP) mice. Tail vein injection of adult rats with aldosterone, 1,2-dioctanoyl-snglycerol (DOG), or 8-(4-chlorophenylthio)-cAMP (cpt-cAMP) induced V-ATPase apical membrane accumulation and extension of V-ATPaselabeled microvilli in clear cells in the caput epididymis but not in the cauda. V-ATPase activity was measured in EGFP-expressing clear cells using the intracellular pH (pH i)-sensing dye seminaphthorhodafluor-5F-5-(and 6)-carboxylic acid, acetoxymethyl ester acetate (SNARF-5F). Aldosterone induced a rapid increase in the rate of Na ϩ -and bicarbonate-independent pH i recovery following an NH4Cl-induced acid load in clear cells isolated from the caput but not the cauda. This effect was abolished by concanamycin A, spironolactone, and chelerythrine but not myristoylated-protein kinase inhibitor (mPKI) or mifepristone. Thus aldosterone increases V-ATPasedependent proton secretion in clear cells in the caput epididymis via MR/NR3C2 and PKC activation. This study, therefore, identifies aldosterone as an active member of the RAAS for the regulation of luminal acidification in the proximal epididymis. aldosterone; nongenomic; epididymis; clear cell; V-ATPase pump THE EPIDIDYMIS IS AN IMPORTANT male reproductive organ involved in the maturation and storage of spermatozoa. The pseudostratified epithelium of the epididymis is composed of numerous cell types, including principal, basal, and clear cells that function in concert to tightly regulate the luminal environment in which sperm transit (51). One major function of clear cells in the epididymis is to acidify the luminal fluid via the vacuolar proton-pumping H ϩ -ATPase (V-ATPase), which is located on the apical membrane (6,7,13,14). Under resting conditions, a large fraction of V-ATPase resides in a subapical pool of vesicles, and upon activation the V-ATPase is trafficked to the apical membrane. This is accompanied by an increase in apical membrane surface area resulting in the formation and elongation of apical microvillar projections. Thus microvilli elongation directly correlates with V-ATPase activity and has been used as a measure of clear cell activation (6,7,19,39,49). The importance of clear cells to male fertility has been demonstrated, as impairment of V-ATPase activity by genetic manipulation or by environmental factor...

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Section: Discussionsupporting

confidence: 93%

Section: Discussionsupporting

confidence: 84%

Section: Discussionmentioning

confidence: 79%

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

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Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Roy

Hill

Ruan

et al. 2013

American Journal of Physiology-Cell Physiology

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Molecular Mechanisms and Regulation of Urinary Acidification

Kurtz

2014

Comprehensive Physiology

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The H+ concentration in human blood is kept within very narrow limits, ~ 40 nM, despite the fact that dietary metabolism generates acid and base loads that are added to the systemic circulation throughout the life of mammals. One of the primary functions of the kidney is to maintain the constancy of systemic acid-base chemistry. The kidney has evolved the capacity to regulate blood acidity by performing three key functions: 1) reabsorb HCO3− that is filtered through the glomeruli to prevent its excretion in the urine; 2) generate a sufficient quantity of new HCO3− to compensate for the loss of HCO3− resulting from dietary metabolic H+ loads and loss of HCO3− in the urea cycle; and 3) excrete HCO3− (or metabolizable organic anions) following a systemic base load. The ability of the kidney to perform these functions requires that various cell types throughout the nephron respond to changes in acid-base chemistry by modulating specific ion transport and/or metabolic processes in a coordinated fashion such that the urine and renal vein chemistry is altered appropriately. The purpose of the article is to provide the interested reader with a broad review of a field that began historically ~ 60 years ago with whole animal studies, and has evolved to where we are currently addressing questions related to kidney acid-base regulation at the single protein structure/function level.

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Aldosterone: Renal Action and Physiological Effects

Johnston

Welch

Cain

et al. 2023

Comprehensive Physiology

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Aldosterone stimulates vacuolar H⁺-ATPase activity in renal acid-secretory intercalated cells mainly via a protein kinase C-dependent pathway

Cited by 46 publications

References 71 publications

Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Molecular Mechanisms and Regulation of Urinary Acidification

Aldosterone: Renal Action and Physiological Effects

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Aldosterone stimulates vacuolar H+-ATPase activity in renal acid-secretory intercalated cells mainly via a protein kinase C-dependent pathway

Cited by 46 publications

References 71 publications

Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Circulating aldosterone induces the apical accumulation of the proton pumping V-ATPase and increases proton secretion in clear cells in the caput epididymis

Molecular Mechanisms and Regulation of Urinary Acidification

Aldosterone: Renal Action and Physiological Effects

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Aldosterone stimulates vacuolar H⁺-ATPase activity in renal acid-secretory intercalated cells mainly via a protein kinase C-dependent pathway