2008 JASN IMPACT FACTOR 7.505	HOME   AUTHOR INFO   EDITORIAL BOARD   SUBSCRIBE   FEEDBACK   ALERTS   HELP
advanced	CURRENT ISSUE	ARCHIVES	JASN Express	ONLINE SUBMISSION

This Article Abstract Full Text (PDF) All Versions of this Article: ASN.2007060693v1 19/5/999    most recent Alert me when this article is cited Alert me if a correction is posted Citation Map Services Email this article to a friend Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Vogt, L. Articles by Navis, G. Search for Related Content PubMed PubMed Citation Articles by Vogt, L. Articles by Navis, G.

Effects of Dietary Sodium and Hydrochlorothiazide on the Antiproteinuric Efficacy of Losartan

Liffert Vogt^*, Femke Waanders^*, Frans Boomsma, Dick de Zeeuw^*, and Gerjan Navis^*,

^* Department of Internal Medicine, Division of Nephrology and Department of Clinical Pharmacology, University Medical Center Groningen, University of Groningen, Groningen, and Department of Internal Medicine, Section of Vascular Pharmacology, Erasmus Medical Center, Rotterdam, Netherlands

Correspondence: Prof. Dr. Gerjan Navis, University Medical Center Groningen, Department of Internal Medicine, Division of Nephrology, Hanzeplein 1, 9713 GZ Groningen, Netherlands. Phone: +31-50-361-2955; Fax: +31-50-361-9310; E-mail: G.J.Navis{at}int.umcg.nl

Received for publication June 21, 2007. Accepted for publication November 6, 2007.

	Abstract

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 
There is large interindividual variability in the antiproteinuric response to blockade of the renin-angiotensin-aldosterone system (RAAS). A low-sodium diet or addition of diuretics enhances the effects of RAAS blockade on proteinuria and BP, but the efficacy of the combination of these interventions is unknown. Therefore, this randomized, double-blind, placebo-controlled trial to determine the separate and combined effects of a low-sodium diet and hydrochlorothiazide (HCT) on proteinuria and BP was performed. In 34 proteinuric patients without diabetes, mean baseline proteinuria was 3.8 g/d, and this was reduced by 22% by a low-sodium diet alone. Losartan monotherapy reduced proteinuria by 30%, and the addition of a low-sodium diet led to a total reduction by 55% and the addition of HCT to 56%. The combined addition of HCT and a low-sodium diet reduced proteinuria by 70% from baseline (all P < 0.05). Reductions in mean arterial pressure showed a similar pattern (all P < 0.05). In addition, individuals who did not demonstrate an antiproteinuric response to losartan monotherapy did respond when a low-sodium diet or a diuretic was added. In conclusion, a low-sodium diet and HCT are equally efficacious in reducing proteinuria and BP when added to a regimen containing losartan and especially seem to benefit individuals who are resistant to RAAS blockade. Combining these interventions in sodium status is an effective method to maximize the antiproteinuric efficacy of RAAS blockade.

	Introduction

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 
Proteinuria is, next to high BP, a major risk factor for progression to ESRD in diabetic and nondiabetic nephropathies. Blockade of the renin-angiotensin-aldosterone system (RAAS) with angiotensin-converting enzyme inhibitors (ACEi) or angiotensin II type 1 receptor (AT1) antagonists protects against progressive renal function loss by reduction of BP and proteinuria.^1–3 However, individual differences in antiproteinuric response to RAAS blockade are large, ranging from zero to complete reduction in proteinuria.⁴ It is interesting that residual proteinuria during RAAS blockade predicts the long-term renal risk for that individual patient.^5,6 Therefore, enhancing the antiproteinuric efficacy is advocated to improve renoprotection.⁷

Sodium restriction and diuretic treatment enhance the responses of proteinuria and BP to RAAS blockade.^8–10 Of note, intervention in sodium status might increase the top of the dosage-response to RAAS blockade.^9,11 Therefore, a larger maximum response can be obtained. In a previous study, we showed that the antiproteinuric response to ACEi was almost completely annihilated by high sodium intake with a blunted BP response as well.^4,9 Antiproteinuric and BP responses could be restored by addition of sodium restriction⁹ or a diuretic.⁴ Presumably, diuretics and sodium restriction enhance the efficacy of RAAS blockade by similar mechanisms—that is, by their effect on volume status. Whether their combination has added effects on the antiproteinuric efficacy of RAAS blockade is unknown. It is also unknown whether patients who are resistant to RAAS blockade have specific benefits of sodium depletion. We therefore examined the effects of sodium restriction, hydrochlorothiazide (HCT), and their combination on proteinuria and BP during losartan in proteinuric patients without diabetes in a randomized, double-blind, placebo-controlled, crossover study.

	RESULTS

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 
Patient Characteristics and Dietary Compliance
We included 34 patients (25 men, 9 women, all Caucasians) with a mean age of 50 yr (range 23–68 yr) and mean (SE) body mass index of 27.5 (0.8) kg/m². Baseline proteinuria was 3.8 (0.4) g/d. Diagnoses were membranous glomerulopathy (7), FSGS (7), membranoproliferative glomerulonephritis (2), minimal-change disease with secondary glomerulosclerosis (2), hypertensive nephropathy (5), IgA nephropathy (5), Alport syndrome (1), and nonconclusive diagnosis (4). One patient could not fulfill the complete protocol (because of psychological distress unrelated to the study medication) and was excluded for further analysis.

During high sodium (HS), mean urinary sodium excretion was 196 (9) mmol/d and during low sodium (LS) was 92 (8) mmol/d (P < 0.001), indicating an adequate dietary compliance with achieved urinary sodium values in the physiologic range (Table 1). LS was accompanied by a lower body weight in all three periods. During losartan, LS reduced body weight significantly more than HCT (Table 1). Urinary urea excretion was significantly lower during LS (Table 1).

View larger version (19K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 1. Intensified intervention in sodium status by combining LS and HCT is an effective tool to maximize the antiproteinuric efficacy of RAAS blockade. Proteinuria (A) and MAP (B) compared with baseline (placebo-HS) after 6-wk treatment with losartan and losartan+HCT combined with HS () and LS (). Data are means (SE). Drug effects in all periods were evaluated by a linear mixed-effect model. Tukey tests were used to localize the differences. *P < 0.05 versus all periods; #P < 0.05 versus same treatment on HS (effect of LS); P < 0.05 versus losartan treatment on same diet (effect of HCT); P < 0.05 versus placebo on same diet.

View larger version (18K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 2. Conservative therapy is equally effective in patients with primary glomerulopathies as in patients with secondary nephropathies. Patients with primary glomerulopathies (membranous glomerulopathy [n = 7], FSGS [n = 7], membranoproliferative glomerulonephritis [n = 2], minimal-change disease with secondary glomerulosclerosis [n = 2], and Alport syndrome [n = 1]) were compared with patients with secondary renal damage (hypertensive nephropathy [n = 5] and IgA nephropathy [n = 5]), excluding the patients with nonconclusive diagnoses (n = 4). It is shown that conservative therapy was equally effective in the patients with primary glomerulopathies (n = 19) as in the patients with IgA or hypertensive nephropathies (n = 10). los, losartan.

To analyze for possible BP dependence of the antiproteinuric response, we entered BP (MAP, SBP, or DBP, respectively) as covariate in our linear effect model; however, no measure of BP contributed significantly to the model. Thus, the overall effects of therapy on proteinuria cannot be explained by the effects on BP. Moreover, baseline proteinuria but not baseline degree of BP predicted outcome in terms of residual proteinuria, with a higher residual proteinuria in patients with a higher baseline proteinuria.

Comparison of Concordance of BP and Proteinuria Responses to LS and HCT When Added to Losartan
To assess whether there are differences in mechanisms of antiproteinuric action between the two different measures of volume depletion, we analyzed the possible concordance of BP and proteinuria responses also separately for the periods with addition of LS or HCT to losartan. There was no concordance between the change in proteinuria and the change in BP when patients were switched from HS to LS during losartan; however, the antiproteinuric response to HCT during losartan correlated significantly with BP effects (R = 0.382, P < 0.05; Figure 3). Furthermore, in all but one patient with a decrease in proteinuria by the addition of HCT to losartan, BP also decreased. In contrast, when LS was added to losartan, in 9 of 29 patients in whom proteinuria decreased by the addition of LS, there was no decrease in BP (Figure 3).

View larger version (12K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 3. The antiproteinuric response of LS during losartan is not dependent on BP, in contrast to the antiproteinuric response of HCT during losartan, which correlates significantly with BP. There was no concordance between the change in proteinuria and the change in MAP when patients were switched from HS to LS during losartan (A), whereas the antiproteinuric response of HCT during losartan correlated significantly with the effects on BP (R = 0.382, P < 0.05; B).

The decrease in proteinuria by LS only was accompanied by lower cholesterol levels. The antiproteinuric effect of losartan during HS and LS was also accompanied by a significant decrease in cholesterol but did not decrease further when HCT was added (Table 2). Triglycerides were unaffected by the various treatments (data not shown).

Serum total protein and albumin levels were not altered by losartan during HS, or by LS as such, but significantly increased when LS, HCT, or their combination were combined with losartan (Table 2).

The addition of HCT to losartan significantly increased uric acid during HS and LS when compared with placebo and losartan. Addition of both HCT and LS increased uric acid levels more than the addition of HCT only (Table 2).

Aldosterone and Renin Levels
Aldosterone and renin significantly increased by the shift from HS to LS during all regimens. Renin but not aldosterone was increased by losartan. HCT significantly increased aldosterone and renin during losartan. Aldosterone and renin were highest during losartan+HCT on LS (Table 2).

The effects of LS and HCT during losartan on aldosterone and renin levels were dissimilar. Addition of LS to losartan significantly increased aldosterone levels more than addition of HCT, whereas HCT increased renin levels more. Accordingly, the aldosterone-renin ratio was not affected by LS during losartan but significantly decreased when HCT was added, suggesting different effects of sodium restriction and HCT on RAAS activity and volume status. During losartan+HCT on LS, the aldosterone-renin ratio was lowest compared with all other treatment periods.

Individual Responses to Interventions
For examination of whether patients who are resistant to RAAS blockade have any specific benefits of sodium depletion, patients were divided into three groups: Resistant (<25% reduction in proteinuria, –10 ± 4%; n = 16), intermediate (25 to 50% reduction, –41 ± 3%; n = 10), and good responders (>50% reduction, –62 ± 3%; n = 7) according to their antiproteinuric response to losartan from baseline (on placebo-HS). Baseline characteristics (age, gender, diagnoses, body mass index, creatinine clearance), dietary compliance, and BP response to losartan did not differ between the groups (Table 3). Baseline proteinuria was similar (Figure 4, top). Antiproteinuric response in resistant and intermediate responders was significantly enhanced by LS or HCT, whereas in good responders, antiproteinuric response did not significantly improve further by LS or HCT (Figure 4, bottom). In all groups, lowest proteinuria was obtained by addition of both LS and HCT to losartan without differences between the groups (Figure 4, top). With this regimen, only one patient remained resistant, five were intermediate, and the number of good responders increased to 26 (²: P < 0.001).

View larger version (19K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 4. In proteinuric patients without diabetes, sodium depletion by LS or a diuretic is specifically beneficial in those who are resistant to RAAS blockade. We examined the effects of LS, HCT, and their combination (LS+HCT) on proteinuria (top) and antiproteinuric response (bottom) during losartan treatment (los). According to their antiproteinuric response to losartan from baseline (BL; on placebo-HS), patients were divided into three groups: Resistant (<25% reduction in proteinuria; n = 16), intermediate (25 to 50% reduction; n = 10), and good responders (>50% reduction; n = 7). Data are means ± SEM. P < 0.05 versus resistant patients on same treatment; P < 0.05 versus losartan on HS.

	DISCUSSION

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

It would be of interest to know whether the added antiproteinuric efficacy of volume depletion was due to lower BP. However, on analysis by the linear mixed-effect model, the added effects on proteinuria could not be explained by the effects on BP. Yet on univariate analysis for the different treatment periods, during HCT the effects on BP correlated to the proteinuria effects. This suggests that other antihypertensives may have had a similar effect, but we have no data to support this assumption.

The reduction of proteinuria by low sodium alone was not observed previously in patients with overt proteinuria as a result of primary glomerular disorders. It is in line with previous data on the effects of low sodium in hypertensive black patients, for whom it was attributed to the concomitant reduction in BP.¹² Moreover, recent data from our own group in healthy young adults demonstrated that sodium restriction significantly reduced urinary albumin excretion within the normal range, with only a borderline effect on BP, suggesting that direct renal effects are not excluded.¹³ Obviously, the effect of sodium restriction alone in our overtly proteinuric patients was not sufficient to refrain from pharmacologic intervention. We did not study the effects of HCT monotherapy, but, in previous studies, HCT alone did not influence proteinuria.^14,15 However, reliable data on this topic are sparse and the aforementioned studies were not corrected for urinary sodium excretion or BP.^14,15

We compared the added effects of low sodium and HCT with losartan for several reasons. First, compliance with sodium restriction can be cumbersome, and it would be convenient if there were an alternative with similar efficacy. Second, there is some evidence that the effects of sodium restriction and HCT might not be equivalent, despite that both act on sodium status. A previous study of patients with severe renal failure demonstrated that thiazides exert their antihypertensive effect by specific vascular changes, rather than by volume depletion.¹⁶ Moreover, in uninephrectomized SHR rats, a model for hypertension and proteinuria, sodium restriction but not diuretic therapy diminished renal hypertrophy, whereas BP was similar.¹⁷ In our study, addition of sodium restriction or HCT to losartan was equally effective in reducing proteinuria. On univariate analysis, the added effect of HCT on proteinuria was associated with BP, whereas this was not the case for the added effect of low sodium, suggesting possible different modes of action. Our data do not allow us to substantiate such mechanisms, and this issue requires further study.

Sodium restriction and HCT induced similar decreases in creatinine clearance during losartan, with the largest decrease during their combination, accompanied by a rise in serum urea. This decrease in GFR did not account for the decrease in proteinuria, as shown by the decrease in protein excretion per milliliter of filtrate, indicating a specific antiproteinuric effect of losartan beyond its effects on renal function. It is well established that during RAAS blockade, shifts in volume status exert distinct effects on renal function, facilitating prerenal failure if volume depletion is severe. Here, the effect on renal function was mild, which is in line with relatively mild interventions in volume status. The clinical significance of the decrease in renal function for long-term outcome cannot be derived from our data, but a decrease in GFR at the onset of treatment generally predicts a subsequent slower decline of renal function, presumably because it reflects a decrease in glomerular pressure.^5,18

Optimization of antiproteinuric treatment strategies can conceivably be obtained by combining diuretic with sodium restriction on top of RAAS blockade, although this approach might be limited by adverse events.¹⁹ Addition of HCT to losartan significantly increased uric acid, renin, and aldosterone. Recent data showed that uric acid is an independent risk factor for the development of ESRD,²⁰ and experimental studies provide evidence that uric acid may be a mediator of renal disease progression.²¹ Moreover, through their profibrotic actions, aldosterone^22–25 and (pro)renin^26–28 can also directly contribute to renal damage. Furthermore, a large meta-analysis in proteinuric patients without diabetes showed that the risk for ESRD was adversely influenced when proteinuria reduction by RAAS blockade was accompanied by pronounced BP reduction.²⁹ This suggests a J curve for BP and long-term renal outcome, with a worse outcome in patients with pronounced BP reduction. However, no adjustment for orthostasis and heart rate was made. Also, patients with lower BP might be those with more severe proteinuria and hypoalbuminemia secondary to the nephrotic syndrome, which could explain their faster progression. The assumption of a J curve for renoprotection is supported by animal studies.³⁰ However, for proteinuria, there is no evidence of a J curve, and the target should be <1 g/d.³¹

Several measures can maximize the effects of RAAS blockade. These include dual blockade³² and intervention in volume status, with sodium restriction, thiazides, loop diuretics, and aldosterone blockade. Esnault et al.⁸ showed in patients with a proteinuria comparable to ours but with a worse renal function that intensified furosemide therapy and avoiding excessive sodium on top of dual RAAS blockade resulted in a further decrease in proteinuria at the expense of a rise in serum creatinine. Our data are in line with theirs and, moreover, show the separate effects of sodium restriction and a diuretic on top of RAAS blockade by AT1 receptor blockade only. Our data suggest that further reduction of proteinuria could have been obtained by further sodium depletion, possibly at the expense of a further rise in serum creatinine. The effects of more vigorous interventions in volume status on top of dual RAAS blockade deserve further investigation. This also applies to volume intervention by aldosterone blockade that may exert specific direct renoprotective effects.^23,24,33,34 We consider it of particular interest that the sodium-depleting measures were effective in improving therapy response in patients with a poor response to monotherapy losartan.

We acknowledge possible weaknesses in our study. Urinary urea excretion was lower during sodium restriction. This could question the specificity of the effect of low sodium, because part of the antiproteinuric effect could be due to lower protein intake. We were unable to detect statistically significant effects of the differences in urinary urea excretion on proteinuria on multivariate analysis, but this does not fully exclude an effect. In a clinical outpatient setting, it is difficult to establish sodium restriction without any effect on protein intake, and vice versa. This was recently demonstrated in patients with stage 4/5 kidney disease in whom BP reduction by a very-low-protein diet was independently related to urinary sodium excretion but not to protein intake.³⁵ In an editorial commentary, it was considered likely that effects of the low-protein diet on BP were due to modification of sodium intake.³⁶ Here, we cannot exclude an effect of altered protein intake on proteinuria, but an effect on BP would not be likely. We studied short-term effects of sodium depletion on top of RAAS blockade on proteinuria; however, short-term reductions in proteinuria predict a slower decline in GFR in nondiabetic nephropathy.³¹ Whether combined sodium depletion is effective in slowing renal function decline has to be confirmed in long-term studies.

We conclude that sodium restriction and diuretic are equally effective in reducing proteinuria and BP when added to AT1 antagonist and are specifically beneficial in patients in whom proteinuria is resistant to RAAS blockade. The largest effect on proteinuria and BP is obtained during their combination. Intensified intervention in sodium status by combining sodium restriction and diuretic is an effective tool to maximize the antiproteinuric efficacy of RAAS blockade.

	CONCISE METHODS

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 
Patients and Protocol
The protocol, which was in accordance with the Declaration of Helsinki, was approved by our local ethical committee and conducted according to the guidelines of good clinical practice. Written informed consent was obtained from each patient before inclusion. Patients were selected from our outpatient renal clinic and were enrolled between March 2004 and June 2006. All patients fulfilled the inclusion criterion of a stable proteinuria >2 g/d and <10 g/d. Only patients with stable renal function (i.e., creatinine clearance >30 ml/min and <6 ml/min per yr decline) and age between 18 and 70 yr were included. Patients with uncontrolled hypertension (MAP >100 mmHg), serum potassium >5.5 mmol/L, cardiovascular disease (myocardial infarction, unstable angina, percutaneous transluminal coronary angioplasty, coronary artery bypass grafting, or stroke within the last 6 mo), contraindication for AT1-antagonist or diuretic use, and/or diabetes were excluded, as well as frequent users of nonsteroidal anti-inflammatory drugs (>2 doses/wk). Additional antihypertensive drugs except for RAAS-blocking agents or diuretics were allowed for BP control. These drugs were kept stable during the study.

Selected patients entered this single-center, prospective, randomized, placebo-controlled, crossover study and were consecutively treated during 6 wk with placebo, losartan (100 mg once daily; Cozaar [Merck & Co. Inc., Whitehouse Station, NJ]), and losartan plus HCT (100/25 mg once daily; Fortzaar [Merck & Co. Inc.]) in random order. Patients were instructed to take the study medication once daily, in the morning, except on study days; on those days, the study drug was not taken before data collection at the hospital (between 8:00 and 9:30 a.m.), allowing BP measurement at trough. At the same time, patients were randomly assigned to either a high-sodium diet (200 mmol Na⁺/d [approximately 4.8 g]) or a low-sodium diet (50 mmol Na⁺/d [approximately 1.2 g]) during 18 wk (three 6-wk periods). After 18 wk, patients changed diet and the three 6-wk periods were repeated.

During the whole study, patients were closely supported by a dietary consultant and were instructed to adhere to a stable protein diet (1.1 g/kg per d) throughout the study. Differences in sodium intake were achieved by replacing sodium-rich products with a low-sodium product of the same product group to remain isocaloric with a similar balance among protein, carbohydrate, and fat. For prevention of concurrent changes in dietary habits, the diets were based on the personal food habits of each patient and fitted to the individual caloric need. Every 2 wk after an overnight fast, patients collected 24-h urine, BP was measured, and blood was sampled to control dietary compliance and to monitor renal function and BP. Collected data at the end of each 6-wk treatment period were used for analysis.

Study Measures
The primary end point was the 24-h proteinuria at the end of each treatment period. Secondary end points were the MAP and serum creatinine, urea, cholesterol, triglycerides, total protein, and albumin. At the end of each period, on the day before every visit, patients collected 24-h urine samples to determine proteinuria and urinary sodium, urea, potassium, and creatinine excretion. Urinary protein was determined using the pyrogallol red-molybdate method. Serum and urinary electrolytes and creatinine and cholesterol, triglycerides, total protein, and albumin levels were determined using an automated multi-analyzer (SMA-C; Technicon, Tarrytown, NY). Aldosterone was measured with a commercially available RIA kit (Diagnostic Products Corp., Los Angeles, CA). Plasma renin activity was measured as described previously with a RIA that detects the amount of angiotensin I produced per hour in the presence of excess angiotensinogen (nanograms of angiotensin I produced per milliliter of plasma per hour). This assay measures the enzymatic activity of active plasma renin in the presence of an excess of its (exogenous) substrate.³⁷ BP was measured under constant conditions, at 1-min intervals by an automatic device (Dinamap; GE Medical systems, Milwaukee, WI), with the patient in semisupine position. After 15 min of measurements, the mean of the last four readings was used for further analysis. MAP was calculated as the sum of one third of SBP and two thirds of the DBP.

Sample Size
We hypothesized that patients would present a mean ± SD proteinuria of 3.5 ± 2 g/d at baseline (placebo on HS). Assuming a reduction of 1.0 ± 0.7 g/d with losartan and an extra reduction of 0.6 ± 0.7 g/d by the addition of HCT or LS, it was estimated that 32 patients had to complete the crossover design sequence to give the study a 90% power to detect a statistically significant difference ( = 0.05). On the basis of an expected dropout rate of 5%, we included 34 patients.

Data Analysis
Results are expressed as mean and SE. Baseline data were obtained after 6-wk placebo treatment with HS. Drug effects in all periods were evaluated using linear mixed-effect models. Tukey tests were used to localize the differences. Statistical significance was assumed at the 5% level of probability. We used SPSS 12.0.1 for Windows (SPSS Inc., Chicago, IL) for all analyses.

	DISCLOSURES

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 
This study was supported by Merck Sharp & Dohme (grant MSGP NETH-15-01).

	Acknowledgments

 
Part of this work (an interim analysis in n = 17) was presented at the annual meeting of the American Society of Nephrology, November 8 through 13, 2005, Philadelphia, PA (J Am Soc Nephrol 16: 2005; 37A).

We thank Corrie Nieuwenhout for skillful assistance at the outpatient clinic.

	Footnotes

 
Published online ahead of print. Publication date available at www.jasn.org.

L.V. and F.W. contributed equally to this work.

	REFERENCES

Top Abstract Introduction RESULTS DISCUSSION CONCISE METHODS DISCLOSURES REFERENCES

 

1. Randomised placebo-controlled trial of effect of ramipril on decline in glomerular filtration rate and risk of terminal renal failure in proteinuric, non-diabetic nephropathy: The GISEN Group (Gruppo Italiano di Studi Epidemiologici in Nefrologia). Lancet 349 : 1857 –1863, 1997[CrossRef][Medline]
2. Brenner BM, Cooper ME, de Zeeuw D, Keane WF, Mitch WE, Parving HH, Remuzzi G, Snapinn SM, Zhang Z, Shahinfar S: Effects of losartan on renal and cardiovascular outcomes in patients with type 2 diabetes and nephropathy. N Engl J Med 345 : 861 –869, 2001[Abstract/Free Full Text]
3. Lewis EJ, Hunsicker LG, Clarke WR, Berl T, Pohl MA, Lewis JB, Ritz E, Atkins RC, Rohde R, Raz I: Renoprotective effect of the angiotensin-receptor antagonist irbesartan in patients with nephropathy due to type 2 diabetes. N Engl J Med 345 : 851 –860, 2001[Abstract/Free Full Text]
4. Buter H, Hemmelder MH, Navis G, de Jong PE, de Zeeuw D: The blunting of the antiproteinuric efficacy of ACE inhibition by high sodium intake can be restored by hydrochlorothiazide. Nephrol Dial Transplant 13 : 1682 –1685, 1998[Abstract/Free Full Text]
5. Apperloo AJ, de Zeeuw D, de Jong PE: Short-term antiproteinuric response to antihypertensive treatment predicts long-term GFR decline in patients with non-diabetic renal disease. Kidney Int Suppl 45 : S174 –S178, 1994[Medline]
6. de Zeeuw D, Ramjit D, Zhang Z, Ribeiro AB, Kurokawa K, Lash JP, Chan J, Remuzzi G, Brenner BM, Shahinfar S: Renal risk and renoprotection among ethnic groups with type 2 diabetic nephropathy: A post hoc analysis of RENAAL. Kidney Int 69 : 1675 –1682, 2006[CrossRef][Medline]
7. Kopple JD: The National Kidney Foundation K/DOQI clinical practice guidelines for dietary protein intake for chronic dialysis patients. Am J Kidney Dis 38 : S68 –S73, 2001[Medline]
8. Esnault VL, Ekhlas A, Delcroix C, Moutel MG, Nguyen JM: Diuretic and enhanced sodium restriction results in improved antiproteinuric response to RAS blocking agents. J Am Soc Nephrol 16 : 474 –481, 2005[Abstract/Free Full Text]
9. Heeg JE, de Jong PE, van der Hem GK, de Zeeuw D: Efficacy and variability of the antiproteinuric effect of ACE inhibition by lisinopril. Kidney Int 36 : 272 –279, 1989[Medline]
10. Houlihan CA, Allen TJ, Baxter AL, Panangiotopoulos S, Casley DJ, Cooper ME, Jerums G: A low-sodium diet potentiates the effects of losartan in type 2 diabetes. Diabetes Care 25 : 663 –671, 2002[Abstract/Free Full Text]
11. Wapstra FH, van Goor H, Navis G, de Jong PE, de Zeeuw D: Antiproteinuric effect predicts renal protection by angiotensin-converting enzyme inhibition in rats with established adriamycin nephrosis. Clin Sci (Lond) 90 : 393 –401, 1996[Medline]
12. Swift PA, Markandu ND, Sagnella GA, He FJ, MacGregor GA: Modest salt reduction reduces blood pressure and urine protein excretion in black hypertensives: A randomized control trial. Hypertension 46 : 308 –312, 2005[Abstract/Free Full Text]
13. Krikken JA, Lely AT, Bakker SJ, Navis G: The effect of a shift in sodium intake on renal hemodynamics is determined by body mass index in healthy young men. Kidney Int 71 : 260 –265, 2007[CrossRef][Medline]
14. Donker AJ, Brentjens JR, van der Hem GK, Arisz L: Treatment of the nephrotic syndrome with indomethacin. Nephron 22 : 374 –381, 1978[Medline]
15. Vogt L, Navis G, Koster J, Manolis AJ, Reid JL, de Zeeuw D: The angiotensin II receptor antagonist telmisartan reduces urinary albumin excretion in patients with isolated systolic hypertension: Results of a randomized, double-blind, placebo-controlled trial. J Hypertens 23 : 2055 –2061, 2005[Medline]
16. Jones B, Nanra RS: Double-blind trial of antihypertensive effect of chlorothiazide in severe renal failure. Lancet 2 : 1258 –1260, 1979[Medline]
17. Benstein JA, Feiner HD, Parker M, Dworkin LD: Superiority of salt restriction over diuretics in reducing renal hypertrophy and injury in uninephrectomized SHR. Am J Physiol 258 : F1675 –F1681, 1990[Medline]
18. Hansen HP, Rossing P, Tarnow L, Nielsen FS, Jensen BR, Parving HH: Increased glomerular filtration rate after withdrawal of long-term antihypertensive treatment in diabetic nephropathy. Kidney Int 47 : 1726 –1731, 1995[Medline]
19. Vogt L, Navis G, de Zeeuw D: Individual titration for maximal blockade of the renin-angiotensin system in proteinuric patients: A feasible strategy? J Am Soc Nephrol 16[Suppl 1] : S53 –S57, 2005
20. Iseki K, Ikemiya Y, Inoue T, Iseki C, Kinjo K, Takishita S: Significance of hyperuricemia as a risk factor for developing ESRD in a screened cohort. Am J Kidney Dis 44 : 642 –650, 2004[CrossRef][Medline]
21. Kang DH, Nakagawa T, Feng L, Watanabe S, Han L, Mazzali M, Truong L, Harris R, Johnson RJ: A role for uric acid in the progression of renal disease. J Am Soc Nephrol 13 : 2888 –2897, 2002[Abstract/Free Full Text]
22. Aldigier JC, Kanjanbuch T, Ma LJ, Brown NJ, Fogo AB: Regression of existing glomerulosclerosis by inhibition of aldosterone. J Am Soc Nephrol 16 : 3306 –3314, 2005[Abstract/Free Full Text]
23. Bianchi S, Bigazzi R, Campese VM: Long-term effects of spironolactone on proteinuria and kidney function in patients with chronic kidney disease. Kidney Int 70 : 2116 –2123, 2006[Medline]
24. Chrysostomou A, Becker G: Spironolactone in addition to ACE inhibition to reduce proteinuria in patients with chronic renal disease. N Engl J Med 345 : 925 –926, 2001[Free Full Text]
25. Miyata K, Rahman M, Shokoji T, Nagai Y, Zhang GX, Sun GP, Kimura S, Yukimura T, Kiyomoto H, Kohno M, Abe Y, Nishiyama A: Aldosterone stimulates reactive oxygen species production through activation of NADPH oxidase in rat mesangial cells. J Am Soc Nephrol 16 : 2906 –2912, 2005[Abstract/Free Full Text]
26. Huang Y, Wongamorntham S, Kasting J, McQuillan D, Owens RT, Yu L, Noble NA, Border W: Renin increases mesangial cell transforming growth factor-beta1 and matrix proteins through receptor-mediated, angiotensin II-independent mechanisms. Kidney Int 69 : 105 –113, 2006[CrossRef][Medline]
27. Huang Y, Noble NA, Zhang J, Xu C, Border WA: Renin-stimulated TGF-beta1 expression is regulated by a mitogen-activated protein kinase in mesangial cells. Kidney Int 72 : 45 –52, 2007[CrossRef][Medline]
28. Nguyen G, Delarue F, Burckle C, Bouzhir L, Giller T, Sraer JD: Pivotal role of the renin/prorenin receptor in angiotensin II production and cellular responses to renin. J Clin Invest 109 : 1417 –1427, 2002[CrossRef][Medline]
29. Jafar TH, Stark PC, Schmid CH, Landa M, Maschio G, de Jong PE, de Zeeuw D, Shahinfar S, Toto R, Levey AS: Progression of chronic kidney disease: The role of blood pressure control, proteinuria, and angiotensin-converting enzyme inhibition—A patient-level meta-analysis. Ann Intern Med 139 : 244 –252, 2003[Abstract/Free Full Text]
30. Hamming I, Navis G, Kocks MJ, van Goor H: ACE inhibition has adverse renal effects during dietary sodium restriction in proteinuric and healthy rats. J Pathol 209 : 129 –139, 2006[CrossRef][Medline]
31. Ruggenenti P, Schieppati A, Remuzzi G: Progression, remission, regression of chronic renal diseases. Lancet 357 : 1601 –1608, 2001[CrossRef][Medline]
32. Nakao N, Yoshimura A, Morita H, Takada M, Kayano T, Ideura T: Combination treatment of angiotensin-II receptor blocker and angiotensin-converting-enzyme inhibitor in non-diabetic renal disease (COOPERATE): A randomised controlled trial. Lancet 361 : 117 –124, 2003[CrossRef][Medline]
33. Kramer AB, van der Meulen EF, Hamming I, van Goor H, Navis G: Effect of combining ACE inhibition with aldosterone blockade on proteinuria and renal damage in experimental nephrosis. Kidney Int 71 : 417 –424, 2007[CrossRef][Medline]
34. Sato A, Hayashi K, Naruse M, Saruta T: Effectiveness of aldosterone blockade in patients with diabetic nephropathy. Hypertension 41 : 64 –68, 2003[Abstract/Free Full Text]
35. Bellizzi V, Di Iorio BR, De Nicola L, Minutolo R, Zamboli P, Trucillo P, Catapano F, Cristofano C, Scalfi L, Conte G: Very low protein diet supplemented with ketoanalogs improves blood pressure control in chronic kidney disease. Kidney Int 71 : 245 –251, 2007[CrossRef][Medline]
36. Weir MR: Is it the low-protein diet or simply the salt restriction? Kidney Int 71 : 188 –190, 2007[CrossRef][Medline]
37. Derkx FH, Tan-Tjiong L, Wenting GJ, Boomsma F, Man in 't Veld AJ, Schalekamp MA: Asynchronous changes in prorenin and renin secretion after captopril in patients with renal artery stenosis. Hypertension 5 : 244 –256, 1983[Abstract/Free Full Text]

This article has been cited by other articles:

				E. I. Ekinci, G. Thomas, D. Thomas, C. Johnson, R. J. MacIsaac, C. A. Houlihan, S. Finch, S. Panagiotopoulos, C. O'Callaghan, and G. Jerums Effects of Salt Supplementation on the Albuminuric Response to Telmisartan With or Without Hydrochlorothiazide Therapy in Hypertensive Patients With Type 2 Diabetes Are Modulated by Habitual Dietary Salt Intake Diabetes Care, August 1, 2009; 32(8): 1398 - 1403. [Abstract] [Full Text] [PDF]

This Article Abstract Full Text (PDF) All Versions of this Article: ASN.2007060693v1 19/5/999    most recent Alert me when this article is cited Alert me if a correction is posted Citation Map Services Email this article to a friend Similar articles in this journal Similar articles in PubMed Alert me to new issues of the journal Download to citation manager Citing Articles Citing Articles via HighWire Citing Articles via Google Scholar Google Scholar Articles by Vogt, L. Articles by Navis, G. Search for Related Content PubMed PubMed Citation Articles by Vogt, L. Articles by Navis, G.