PPARγ activation enhances cell surface ENaCα via up‐regulation of SGK1 in human collecting duct cells

Hong, Guizhu; Lockhart, Andrew; Davis, Bill; Rahmoune, Hassan; Baker, Sharon F.; Liang, Ye; Thompson, Paul; Shou, Yaping; O’Shaughnessy, Kevin M.; Ronco, Pierre; Brown, John

doi:10.1096/fj.03-0181fje

Cited by 101 publications

(112 citation statements)

References 38 publications

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“…The latter were in the lower micromolar range (10-15 μM), which is comparable to levels measured in volunteers after oral ingestion of 30 mg pioglitazone (3 μM; [44]). At those concentrations, pioglitazone does increase extracellular fluid volume, as previously shown for PPARγ agonists [18,22,49].…”

Section: Discussionsupporting

confidence: 78%

“…The use of the PPARγ agonists has, however, been impeded by their volume retaining properties [18,22,49]. In patients with congestive heart failure (CHF), treatment with PPARγ agonists was associated with decompensation and occurrence of pulmonary edema [35].…”

Section: Introductionmentioning

confidence: 99%

“…On the one hand, PPARγ agonists were found to upregulate mRNA levels of SCNN1G encoding for the gamma subunit of ENaC in a mouse inner medullary collecting duct cell line [19]. On the other hand PPARγ agonists have been shown to stimulate the transcription of the serum and glucocorticoid-inducible kinase SGK1 [22], which, in turn, was suggested to enhance the surface expression of ENaCα [22]. In three well-established cell culture models of the renal principal cell type, PPARγ agonists did not alter basal or insulin-stimulated ENaC activity and may thus be effective through additional mechanisms [36], which, at least in theory, could be similarly sensitive to SGK1.…”

Section: Introductionmentioning

confidence: 99%

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Lack of the serum and glucocorticoid-inducible kinase SGK1 attenuates the volume retention after treatment with the PPARγ agonist pioglitazone

Artunc

Sandulache

Nasir

et al. 2008

Pflugers Arch - Eur J Physiol

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PPARγ-agonists enhance insulin sensitivity and improve glucose utilization in diabetic patients. Adverse effects of PPARγ-agonists include volume retention and edema formation. Recent observations pointed to the ability of PPARγ agonists to enhance transcription of the serum and glucocorticoid-inducible kinase SGK1, a kinase that is genomically upregulated by mineralocorticoids and stimulates various renal channels and transporters including the renal epithelial Na + channel ENaC. SGK1 has been proposed to mediate the volume retention after treatment with PPARγ agonists. To test this hypothesis, food containing the PPARγ agonist pioglitazone (0.02%, i.e., approximately 25 mg/kg bw/day) was administered to gene-targeted mice lacking SGK1 (sgk1 −/− , n=12) and their wild-type littermates (sgk1 +/+ , n=12). According to in situ hybridization, quantitative reverse transcriptase-polymerase chain reaction (RT-PCR) and immunofluorescence, treatment with pioglitazone significantly increased renal SGK1 mRNA and protein expression in sgk1 +/+ mice. The treatment increased body weight significantly in both, sgk1 +/+ mice (+2.2±0.3 g) and sgk −/− mice (+1.3±0.2 g), and decreased hematocrit significantly in sgk1 +/+ mice (−6.5±1.0%) and sgk1 −/− mice (−3.1±0.6%). Both effects were significantly (p<0.05) more pronounced in sgk1 +/+ mice. According to Evans Blue

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Section: Discussionsupporting

confidence: 78%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Lack of the serum and glucocorticoid-inducible kinase SGK1 attenuates the volume retention after treatment with the PPARγ agonist pioglitazone

Artunc

Sandulache

Nasir

et al. 2008

Pflugers Arch - Eur J Physiol

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“…This notion is supported by several lines of direct and indirect evidence from previous studies. First, in a cultured human cortical CD cell line, PPAR␥ agonists increase levels of cell surface ENaC␣, paralleled by stimulation of gene expression of serum and glucocorticoid regulated kinase 1 (SGK1), a key mediator of aldosterone activation of ENaC (29). Second, a PPAR␥ ligand, GI262570, increased expressions of ENaC␣, SGK1, and Na-K-ATPase␣ in the renal medulla (26).…”

Section: Discussionmentioning

confidence: 99%

Collecting duct-specific deletion of peroxisome proliferator-activated receptor γ blocks thiazolidinedione-induced fluid retention

Zhang

Kohan

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

311

264

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The peroxisome proliferator-activated receptor subtype ␥ (PPAR␥) ligands, namely the synthetic insulin-sensitizing thiazolidinedione (TZD) compounds, have demonstrated great potential in the treatment of type II diabetes. However, their clinical applicability is limited by a common and serious side effect of edema. To address the mechanism of TZD-induced edema, we generated mice with collecting duct (CD)-specific disruption of the PPAR␥ gene. We found that mice with CD knockout of this receptor were resistant to the rosiglitazone-(RGZ) induced increases in body weight and plasma volume expansion found in control mice expressing PPAR␥ in the CD. RGZ reduced urinary sodium excretion in control and not in conditional knockout mice. Furthermore, RGZ stimulated sodium transport in primary cultures of CD cells expressing PPAR␥ and not in cells lacking this receptor. These findings demonstrate a PPAR␥-dependent pathway in regulation of sodium transport in the CD that underlies TZD-induced fluid retention.roziglitazone ͉ Cre recombinase ͉ Evans blue technique T hiazolidinediones (TZDs), synthetic insulin-sensitizing drugs that include troglitazone, pioglitazone, and rosiglitazone (RGZ), are highly effective in the treatment of type II diabetes. TZDs are believed to mediate their antidiabetic effect via activation of peroxisome proliferator-activated receptor ␥ (PPAR␥) (1). In addition to lowering blood glucose, these drugs also benefit cardiovascular parameters, such as blood pressure and endothelial function (2, 3). However, fluid retention, presented as rapid weight gain, and peripheral and pulmonary edema have emerged as the most common and serious side effects of TZDs (4-6). Global awareness of this side effect has increased as a result of the growing number of reported cases. In a recent issue of Circulation (7), the American Heart Association and American Diabetes Association jointly issued a Consensus Statement commenting on the safety of TZD as related to edema. The mechanisms of fluid retention in patients treated with TZDs are poorly understood and may involve a number of factors, including reduction of urinary sodium excretion (8), alteration of endothelial permeability (9), increased sympathetic nervous system activity (10), or altered interstitial ion transport (11). To evaluate the relative contributions of these individual mechanisms, tissue-or cell-type-specific approaches are needed in carefully designed studies.PPARs are a group of zinc finger-containing transcription factors, representing a family of the nuclear hormone receptor gene superfamily. To date, three subtypes of PPARs encoded by different genes have been described from several species: PPAR␣, -␤͞␦, and -␥ (12, 13). They share a high degree of similarity in their overall amino acid sequences, particularly in the DNA-binding domain (14). The three isoforms of the PPARs heterodimerize with retinoid X receptor, bind to the same peroxisome proliferatorresponsive element in the promoter regions of their target genes, and modulate gene transcripti...

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“…The mechanisms of action behind the fluid retention with TZDs (e.g., cardiac cause or drug interaction with receptors on sodium channels) remain unclear, although it has been suggested that peroxisome proliferator-activated receptor-␥ may regulate sodium reabsorption in the cortical collecting ducts (segments of the nephron involved in regulation of sodium and water homeostasis) via stimulation of epithelial sodium channel activity (22). The long-term study of pioglitazone use and heart failure, funded by the American Diabetes Association (18), argues against the possibility that TZDs cause heart failure.…”

Section: Edemamentioning

confidence: 99%

Pioglitazone Use and Heart Failure in Patients With Type 2 Diabetes and Preexisting Cardiovascular Disease

Charbonnel²,

et al. 2007

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OBJECTIVE— PROspective pioglitAzone Clinical Trial In macroVascular Events (PROactive) enrolled patients with type 2 diabetes and preexisting cardiovascular disease. These patients were at high risk for heart failure, so any therapeutic benefit could potentially be offset by risk of associated heart failure mortality. We analyzed the heart failure cases to assess the effects of treatment on morbidity and mortality after reports of serious heart failure. RESEARCH DESIGN AND METHODS— PROactive was an outcome study in 5,238 patients randomized to pioglitazone or placebo. Patients with New York Heart Association Class II–IV heart failure at screening were excluded. A serious adverse event of heart failure was defined as heart failure that required hospitalization or prolonged a hospitalization stay, was fatal or life threatening, or resulted in persistent significant disability or incapacity. Heart failure risk was evaluated by multivariate regression. RESULTS— More pioglitazone (5.7%) than placebo patients (4.1%) had a serious heart failure event during the study (P = 0.007). However, mortality due to heart failure was similar (25 of 2,605 [0.96%] for pioglitazone vs. 22 of 2,633 [0.84%] for placebo; P = 0.639). Among patients with a serious heart failure event, subsequent all-cause mortality was proportionately lower with pioglitazone (40 of 149 [26.8%] vs. 37 of 108 [34.3%] with placebo; P = 0.1338). Proportionately fewer pioglitazone patients with serious heart failure went on to have an event in the primary (47.7% with pioglitazone vs. 57.4% with placebo; P = 0.0593) or main secondary end point (34.9% with pioglitazone vs. 47.2% with placebo; P = 0.025). CONCLUSIONS— Although the incidence of serious heart failure was increased with pioglitazone versus placebo in the total PROactive population of patients with type 2 diabetes and macrovascular disease, subsequent mortality or morbidity was not increased in patients with serious heart failure.

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PPARγ activation enhances cell surface ENaCα via up‐regulation of SGK1 in human collecting duct cells

Cited by 101 publications

References 38 publications

Lack of the serum and glucocorticoid-inducible kinase SGK1 attenuates the volume retention after treatment with the PPARγ agonist pioglitazone

Lack of the serum and glucocorticoid-inducible kinase SGK1 attenuates the volume retention after treatment with the PPARγ agonist pioglitazone

Collecting duct-specific deletion of peroxisome proliferator-activated receptor γ blocks thiazolidinedione-induced fluid retention

Pioglitazone Use and Heart Failure in Patients With Type 2 Diabetes and Preexisting Cardiovascular Disease

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