Proteinuria patterns and their association with subsequent end-stage renal disease in IgA nephropathy
James V. Donadio1,,
Erik J. Bergstralh2,
Joseph P. Grande3 and
Diana M. Rademcher2
1 Division of Nephrology, Department of Internal Medicine,
2 Section of Biostatistics and
3 Division of Anatomic Pathology, Department of Laboratory Medicine and Pathology, Mayo Clinic and Foundation, Rochester, MN, USA
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Abstract
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Background. Proteinuria (UP) >1.0 g/24 h at diagnosis is a well-known indicator of progressive renal disease in patients with IgA nephropathy (IgAN). To determine if persistent UP is a more sensitive marker for later progression of IgAN, the hypothesis was tested that the prior level and trend (slope) in UP for 1 year was better at predicting later end-stage renal disease (ESRD) (dialysis or transplant) than a current 24-h UP, serum creatinine (SC), SC slope, hypertension, or total glomerular histopathological score on index renal biopsy in an observational study of 154 high-risk patients enrolled in two clinical trials (IgAN 1, IgAN 2).
Methods. Measurements of 24-h UP and SC were made at time 0, 6 weeks, 6 months and 1 year in all patients, who were then followed for an additional 5.76 years and 1.63 years in the two studies, respectively. The Cox proportional hazards model was used to identify predictors of ESRD following the 1-year visit.
Results. Adjusting only for randomized treatment, nearly all UP variables (number of high readings, 1-year level, slopes), SC at 1 year, and SC trends (slopes) over the prior year were significantly associated with subsequent ESRD (all P values <0.05) in both studies. However, among the UP variables, the 1-year readings had the strongest association with ESRD in IgAN 1 (hazard ratio (HR), 95% CI, for a 1g increase: 1.5, 1.2,1.9), and the second strongest association (similar to UP trends) in IgAN 2 (1.4, 1.2,1.6). Males had lower rates of ESRD in both studies (IgAN 1 HR: 0.5, 0.2,1.2, P=0.11; IgAN 2 HR: 0.2, 0.1,0.6, P=0.002). In the multivariate analyses that examined all clinical and histological variables, 1-year levels of 24-h UP and SC, and female gender were independently associated with subsequent ESRD.
Conclusion. In a high-risk patient with IgAN, the current 24-h UP and SC measurements are as good predictors of subsequent ESRD as UP and SC trends and levels over the prior year. Additionally, it appears that females have poorer outcomes than males.
Keywords: IgA nephropathy; prognosis; proteinuria
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Introduction
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At the time of renal biopsy diagnosis, proteinuria is a well-known indicator of progressive renal disease in patients with IgA nephropathy (IgAN). Among the risk factors examined in clinicopathological studies, increasing levels of urine protein (UP) >1.0 g/24 h is strongly associated with later development of renal failure [1]. Persistent proteinuria exceeding 1.0 g/24 h was an independent predictor of subsequent renal progression in a recently reported large series of patients with IgAN followed for 10 years or more [2].
In idiopathic membranous nephropathy, another glomerulopathy associated with high levels of UP, Pei et al. [3] showed that the highest sustained, 6-month period of proteinuria was an independent predictor of renal progression. This semiquantitative, predictive model was validated in an analysis of independent data from two other series of patients with membranous nephropathy [4]. In this study, it was also pointed out that, ideally, the defined time period of increased UP should be early enough in the clinical course of a patient to allow for a timely discussion between doctor and patient about prognosis, and for the physician to prescribe therapies that may slow progression of the renal disease. For example, the time from renal biopsy diagnosis to the start of the worst 6 months of proteinuria occurred between 1 and 2 years in 7285% of the three groups of patients studied [4].
To determine if persistent proteinuria is an early, sensitive and independent marker for later progression of IgAN, the hypothesis was tested that the prior trend in UP for 1-year was better at predicting subsequent renal failure events than a current UP, serum creatinine, or other commonly used predictors (e.g. age, gender, blood pressure measurement of the day, or total glomerular histopathological score) in an observational study based on post-hoc analysis of two patient cohorts who participated in randomized clinical trials that tested the efficacy of omega-3 polyunsaturated fatty acids (
-3 PUFA) [57].
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Methods
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Patients
In this review, the first group (IgAN 1) of 106 patients participated in a randomized, placebo-controlled, double-blind trial [5,6], and the second group (IgAN 2) of 73 patients took part in a randomized, open-label,
-3 PUFA 2-dose comparative design [7]. The study period for the first trial extended from June 1988 to December 1993, and for the second trial from September 1995 to January 2000. In both studies, patients were followed for a minimum of 2 years unless they developed a study end point or became non-compliant. Long-term, off-study follow-up data for serum creatinine levels and end-stage renal disease (ESRD) was collected for IgAN 1.
Study design
As the two trials had differing enrolment criteria regarding UP levels (IgAN 1,
1.0 g/24 h; IgAN 2, any amount), differing treatments (IgAN 1,
-3 PUFA vs placebo; IgAN 2, low vs high-dose
-3 PUFA), and differing lengths of follow-up beyond 1 year (IgAN 1, 5.76 year, median; IgAN 2, 1.63 year, median), we felt it prudent to perform separate analyses for each trial.
In order to allow for a reasonable number of prior UP readings and an adequate number of subsequent renal events, all analyses were based on the patients who were alive at 1 year without prior ESRD. All patients in both trials had four prior UP and serum creatinine measurements taken at scheduled visits (baseline, 6 weeks, 6 month and 1 year). One or two (average taken if two) 24-h UP determinations were made at each scheduled visit. Proteinuria levels were measured with Pyrogallol Red Molybdate Reagent (Waco Pure Chemicals Industries Ltd, Osaka, Japan) using a technique adapted from the method described by Yoshimoto et al. [8]. Missing values were imputed using within-patient linear regression analysis for 15 UP readings (in 15 patients) out of a total of 616 readings.
Statistical analysis
The focus of the data analysis was to address the predictive ability of a current (1-year trial visit) UP measurement relative both to changes in proteinuria over the past year, and to the number (04) of high (>500, >1,000, >1,500, >2,000, >2,500 or >3,000 mg/24 h) UP levels measured over the past year. Changes in UP and serum creatinine were based on slopes from within patient linear regression analyses using the four prior readings. The linearity assumption seemed tenable for the relatively short period of 1 year.
Time from the 1-year trial visits in IgAN 1 and IgAN 2 to the end point of ESRD, was estimated using the KaplanMeier method [9]. Due to differing follow-up, the percentage (Kaplan-Meier) of patients free of ESRD and the standard error was summarized at 6 years (after the 1-year visit) for the IgAN 1 trial, and at 2 years (also after the 1-year visit) for the IgAN 2 trial. The univariate association of factors (analysed as a linear trend in the log hazard rate for continuous factors) with time to ESRD was assessed using the Cox proportional hazards model [10]. Results based on the Cox model are presented using hazard ratios (HR) and 95% confidence intervals. Multivariate analyses were done using stepwise regression (Cox model) analysis in an attempt to identify which variables were most important in predicting subsequent ESRD. In the first analysis only the UP variables (adjusted for randomized treatment group) were included. This was followed by an analysis including all variables (adjusted for treatment) including serum creatinine variables (1-year measurement and slope), presence of hypertension at 1 year, and total glomerular histopathological score on the index renal biopsy. All renal biopsies were performed at various intervals preceding the trials, and the assumption was made that there was no change in the pathology when the biopsy scores were applied to the Cox model. In a previous study of 148 patients with IgAN, total glomerular score, derived from the extent of mesangial cell proliferation, matrix increase, capillary loop narrowing or disruption, glomerular sclerosis, cellular crescents and fibrous adhesions, was an independent predictor of adverse outcome [1]. All tests were 2-sided at alpha level 0.05.
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Results
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There were 91 patients in IgAN 1 (74% male) and 63 patients in IgAN 2 (83% male) who were alive after 1-year of follow-up and had not reached ESRD in their respective trials. There were 18 ESRD events after 1 year in IgAN 1, and 14 ESRD events after 1 year in IgAN 2.
There was a wide distribution of 24-h UP levels and slopes over the prior year in both study cohorts with the most favourable changes, i.e. a reduction of 500 mg/24 h or greater (slope) occurring in the IgAN 1 group (Table 1
). Sixty to ninety per cent of patients in both groups had had 75100% (3 or 4) of their UP readings above the 500 and 1,000 mg/24 h levels during the previous year (Table 2
). The percentages of patients having 34 readings declined with an increase in UP levels. Seventy-seven out of the 91 patients (85%) in IgAN 1, and 25/63 patients (40%) in IgAN 2 had serum creatinine <2 mg/dl at 1 year. Slopes in serum creatinine were more positive, i.e.
0.30 mg/dl/year, in more IgAN 2 patients, indicating worsening renal function, compared with IgAN 1 (Table 1
). This reflects a better baseline renal function in IgAN 1 patients [5]. Due to the study design, eligibility serum creatinine entry levels in IgAN 1 had to be <3.0 mg/dl [5], and in IgAN 2 eligible serum creatinine levels ranged from 1.5 to 4.9 mg/dl [7]. The presence of uncontrolled hypertension at 1 year and total glomerular histopathological scores were similar in the two groups (Table 1
). Angiotensin-converting enzyme (ACE) inhibitor use at 1 year was documented in 53% of IgAN 1 patients and 78% of IgAN 2 patients.
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Table 1. Urine protein, serum creatinine, hypertension and glomerular score in patients with a 1-year visit and no prior ESRD
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Urine protein levels measured at 1 year (Figures 1A
and B
) and slopes over the prior 1 year (Figures 2A
and B
) were significantly associated with subsequent ESRD following the 1-year visit in both IgAN 1 (HR, 95% CI, for a 1 g increase: 1.5, 1.2,1.9) and IgAN 2 (1.4, 1.2,1.6) (Table 3
). Higher frequencies of readings above all pre-selected UP cut-off points were also significantly associated with later ESRD (Table 3
).

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Fig. 1. 24-h UP levels at 1 year were significantly associated with subsequent ESRD after 1 year on study in (A) IgAN 1 (P<0.001, linear trend) and (B) IgAN 2 (P<0.001, linear trend).
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Fig. 2. 24-h UP trends (slopes) over the prior year were significantly associated with later ESRD after 1-year of study in (A) IgAN 1 (P=0.007, linear trend) and (B) IgAN 2 (P=0.01, linear trend).
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Table 3. HR and 2 of individual predictors of ESRD after 1 year of study adjusted for treatment effects using the Cox model
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Serum creatinine measurements at 1 year (Figures 3A
and B
) and slopes over the prior 1 year (Figures 4A
and B
) were strongly associated with the subsequent development of ESRD after the 1-year visit in both study groups (Table 3
).

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Fig. 3. Serum creatinine concentrations at 1-year were significantly associated with subsequent ESRD in (A) IgAN 1 (P<0.001, linear trend) and (B) IgAN 2 (P<0.001, linear trend).
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Fig. 4. Serum creatinine trends (slopes) over the prior year were significantly associated with subsequent ESRD in (A) IgAN 1 (P<0.001, linear trend) and (B) IgAN 2 (P<0.001, linear trend).
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Hypertension and ACE inhibitor use at 1 year were not associated with later ESRD, and higher total glomerular scores were associated with ESRD events in IgAN 1 only. Six-year ESRD-free survival was 93, 75 and 62%, for glomerular scores of 14, 57 and 811, respectively (P<0.001). Males had lower rates of ESRD in both studies (IgAN 1 HR: 0.5, 0.2,1.2, P=0.11; IgAN 2 HR: 0.2, 0.1,0.6, P=0.002) (Table 3
). At 2 years, ESRD-free survival was 84±6% for males and 46±17% for females in IgAN 2.
In the multivariate analysis for IgAN 1, adjusting only for treatment, the strongest predictor (
2 to enter stepwise model) of subsequent ESRD was the serum creatinine value at 1 year, followed by the serum creatinine slope and the UP value at 1 year (Table 3
). Among the UP variables, the only significant independent (stepwise regression) predictor of ESRD was the UP value at 1 year. Using all the variables listed in Table 3
, serum creatinine concentration at 1 year, UP measurement at 1 year and gender (females at higher risk) were selected as independent predictors of ESRD (all three P-values <0.001).
In IgAN 2, adjusting only for treatment, the strongest predictor of subsequent ESRD was the serum creatinine slope, followed by the serum creatinine concentration at 1 year, and the UP value at 1 year (Table 3
). Among UP variables, the only significant independent (stepwise regression) predictor of ESRD was the UP value at 1 year, which is consistent with the findings in IgAN 1. Using all the variables listed in Table 3
, serum creatinine slope (P<0.001), UP slope (P=0.002) and female gender (P=0.001) were selected as independent predictors of ESRD (model
2=49.7). A model including gender, UP at 1 year and serum creatinine at 1 year (the model selected for IgAN 1) had an almost identical predictive power (model
2=46.4).
A pooled analysis combining IgAN 1 and IgAN 2 found similar results.
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Discussion
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A current assessment of 24-h UP excretion and serum creatinine concentration gave either better or equivalent prognostic information over UP trends on the subsequent development of ESRD in separate analyses of two cohorts of patients with IgAN who were enrolled in prospective clinical trials that tested the efficacy of
-3 PUFA and involved long-term follow-up [57]. The one-time serum creatinine and UP values at 1-year study visits in both study groups were independently associated with subsequent renal failure outcomes. In multivariate analysis, females patients appeared to have poorer outcomes in both cohorts. Total glomerular histopathological scores of index renal biopsies were univariately significant for one cohort.
In the current study, we directly compare the relative value of a single 24-h UP determination vs trends in UP excretion over time in ascertaining the risk of renal disease progression. Although several recent studies have established that baseline proteinuria and serum creatinine are strong predictors of subsequent GFR decline and progression to ESRD [11], the predictive value of a single baseline UP excretion determination vs trends in proteinuria obtained by repeated measurements over time has not been previously assessed. In a high-risk patient with IgAN, this study shows that knowing a 1-year history of proteinuria, which is often not available for the clinician's review, is no more useful a clinical predictor of subsequent adverse renal outcome than is having the clinical information of proteinuria and renal function of a single day. These findings are based on prospective studies in which patients had four scheduled study visits over the first year of study enrolment. In practice, many patients will not have had this systematic evaluation of their clinical course. Thus, the practical value of the findings in the present study indicates that a current 24-h measurement of proteinuria and serum creatinine will provide the best information required to assess a clinical course and prescribe appropriate therapies.
These findings are at variance with those of Kobayashi et al. [2] who reported that persistent proteinuria exceeding 1,000 mg/24 h was the most reliable, independent predictor of long-term prognosis in Japanese patients with IgAN followed for 10 years or more. Detailed information concerning the methodology and analysis of a number of clinical variables related to outcome is not available as this study was published in abstract form only. There are no other prospective longitudinal studies examining persistent proteinuria as a risk factor in IgAN; only retrospective clinicopathological studies showing that baseline proteinuria is associated with later development of adverse renal outcomes [1].
It is important to define the clinical setting in which persistent proteinuria occurs. A protein excretion of less than 4 g/day is seen in both interstitial and glomerular diseases, whereas an excretion rate greater than 4 g/day is almost invariably the result of glomerular disease. In general terms, in glomerulonephritis associated with the nephrotic syndrome, a progressive decline in proteinuria to less than 2 g/day (or less) is associated with a favourable prognostic outlook, whether the reduction occurs spontaneously or in response to treatment [12].
In idiopathic membranous nephropathy, another primary glomerular disease associated usually with nephrotic-range proteinuria, Pei et al. [3] constructed a predictive model for renal progression using a 6-month period of the highest amount of UP as the best predictor. Membranous nephropathy differs from IgAN in that it is associated with more massive proteinuria, whereas in IgAN, UP excretion averages between 1000 and 3000 mg/24 h and is quite variable, as reported in most study cohorts including the two study groups that were examined in the present study [1,57]. It is not surprising, therefore, that the longitudinal determination of proteinuria that was carried out in the present study did not have a strong, independent predictive value in estimating later progressive renal failure.
However, a reduction in proteinuria is considered by many investigators to be the hallmark for determining treatment effectiveness in preserving renal function in non-diabetic renal disease. This is exemplified in a recent meta-analysis of 11 randomized clinical trials testing the efficacy of ACE inhibitors in non-diabetic renal disease [13]. This study showed that higher levels of baseline and current levels of UP were associated with progressive renal disease in both ACE inhibitor and control groups. Patients were not analysed according to the causes of their renal diseases.
Therapeutic interventions using a variety of pharmacological agents in IgAN have had varying effects on UP [14]. In three randomized clinical trials [1517] and a large cohort retrospective study [18], a variety of ACE inhibitors has been shown to modestly lower UP in patients with IgAN. However, no improvement in renal function was demonstrated. Angiotensin receptor antagonists and ACE inhibitors reduced proteinuria equally in two short-term trials [19,20], and the combination was additive in one of these studies [20]. In a randomized clinical trial, treatment with corticosteroids was shown to lower proteinuria 50% after 6 months and to reduce renal progression by 36% after 5 years [21]. In three randomized trials testing the efficacy of
-3 PUFA there was an inconsistent reduction in proteinuria [57,22,23] raising concerns about the long-term efficacy of
-3 PUFA [14].
The present observational study was carried out to determine the value of UP trends as a predictor of later adverse renal outcome and was based on two study cohorts that involved clinical trials testing efficacy of
-3 PUFA. In the first placebo-controlled, randomized, 2-year trial (IgAN 1), despite the differences in renal end points favouring the
-3 PUFA-treated group, the overall reduction in UP (based on slopes) was modest and not significantly different between the
-3 PUFA and placebo groups, nor between normotensive and hypertensive patients, the latter having been treated primarily with an ACE inhibitor [5,6]. However, the magnitude of the reduction in proteinuria was similar to that achieved in studies reporting the effects of ACE inhibitors in patients with IgAN [1518], the majority of whom had UP levels in the sub-nephrotic range, i.e. between 1000 and 3000 mg/24 h, as was the case with our patients. In the second study, an open-label,
-3 PUFA two-dose, comparative trial (IgAN 2), there was a modest decline in proteinuria over time and evidence of a slowing in the rate of renal function loss in high-risk patients with moderately advanced disease [7].
In high-risk patients with IgAN, the predictive power of UP excretion at one point in time is greater than any potential effects of therapeutic intervention, whether ACE inhibition or
-3 PUFA.
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Acknowledgments
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The authors acknowledge Cherish Grabau for secretarial support. This work was supported in part by a research grant from Mayo Foundation, Rochester, MN, USA.
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Notes
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Correspondence and offprint requests to: James V. Donadio MD, Emeritus Staff, Mayo Clinic, 200 First Street South West, Stabile 722, Rochester, MN 559050001, USA. Email: donadio.james{at}mayo.edu 
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Received for publication: 13. 8.01
Accepted in revised form: 31. 1.02