Figures
Abstract
Beneficial effects of omega-3 fatty acid (O3FA) supplementation in a wide range of disease condition have been well studied. However, there is limited information regarding the effects of O3FAs on chronic kidney disease (CKD), especially in diabetic nephropathy (DN) with hypertriglyceridemia. We investigate whether O3FA supplementation could help maintain renal function in patients with diabetes and hypertriglyceridemia. Total 344 type 2 diabetic patients with a history of O3FA supplementation for managing hypertriglyceridemia were included. Reduction in urine albumin to creatinine ratio (ACR) and glomerular filtrate rate (GFR) were examined. Subgroup analyses were stratified according to the daily O3FA doses. Serum total cholesterol, triglyceride, and urine ACR significantly reduced after O3FA supplementation. Overall, 172 (50.0%) patients did not experience renal function loss, and 125 (36.3%) patients had a GFR with a positive slope. The patients treated with O3FAs at 4g/day showed greater maintenance in renal function than those treated with lower dosages (p < 0.001). This dose dependent effect remains significant after adjustment for multiple variables. O3FA supplementation in diabetic patients with hypertriglyceridemia shows benefits of reducing albuminuria and maintaining renal function. The effects are dependent on the dose of daily O3FA supplementation.
Citation: Han E, Yun Y, Kim G, Lee Y-h, Wang HJ, Lee B-W, et al. (2016) Effects of Omega-3 Fatty Acid Supplementation on Diabetic Nephropathy Progression in Patients with Diabetes and Hypertriglyceridemia. PLoS ONE 11(5): e0154683. https://doi.org/10.1371/journal.pone.0154683
Editor: Wolf-Hagen Schunck, Max Delbrueck Center for Molecular Medicine, GERMANY
Received: November 2, 2015; Accepted: April 18, 2016; Published: May 2, 2016
Copyright: © 2016 Han et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
Data Availability: All relevant data are within the paper and its Supporting Information files.
Funding: The authors have no support or funding to report.
Competing interests: The authors have declared that no competing interests exist.
Introduction
Chronic kidney disease (CKD) is defined as kidney dysfunction present for > 3 months, with a glomerular filtration rate (GFR) < 60 mL/min/1.73 m2 [1]. Many studies have reported that both lower GFR and greater albuminuria are independently related to the rates of end-stage renal disease (ESRD), cardiovascular events, and mortality. Albuminuria severity is strongly predictive of poor outcomes at all levels of GFR. More than 40% of subjects with type 2 diabetes mellitus (DM) develop diabetic nephropathy (DN) [2], which has become the leading cause of ESRD [3]. DN is characterized by abnormal urinary albumin excretion progressing from microalbuminuria (30–300 μg/min) to macroalbuminuria (> 300 μg/min) [1]. In addition, GFR is known to decrease with age, at less than 1 ml/min/1.73 m2/year, in healthy individuals [4]; this is accelerated in DN to 5.2 ml/min/1.73 m2/year [5]. Nevertheless, early screening and limited intervention can prevent or delay DN progression in diabetic patients with microalbuminuria [6].
Omega-3 fatty acids (O3FAs) are polyunsaturated fatty acids (PUFAs) derived from fish oil; the three types are α-linoleic acid (ALA), eicosapentaenoic acid (EPA) and docosahexaenoic acid (DHA). These are essential fatty acids, and small amounts of dietary O3FAs enable normal growth. O3FAs also reduce blood triglyceride levels [7–9]. Although somewhat controversial, regular O3FA supplementation may reduce the risks of myocardial infarction and sudden cardiac death [10]. Some evidence suggests that it may improve blood circulation; increase the breakdown of fibrin, a compound involved in clot and scar formation; and reduce blood pressure and heart rate [11–13]. Hypertension is a major risk factor for CKD development, and it is expected that O3FAs could inhibit CKD progression due to their anti-hypertensive effect.
Numerous studies have evaluated the potential beneficial effects of O3FAs on inflammatory, autoimmune, and renal diseases [14, 15]. O3FAs can reduce proteinuria in patients with chronic glomerular disease and slow immunoglobulin A (IgA) nephropathy [16]. Due to their anti-inflammatory effects, O3FAs have been suggested to protect against kidney damage. An animal model study showed that O3FA supplementation reduced renal inflammation and fibrosis [17]. In addition, a large community-based cohort study reported that increased dietary intake of long-chain n-3 PUFA and fish reduces CKD prevalence [18].
However, there is limited information regarding the effects of O3FAs on CKD, especially in patients with DN. The role of O3FAs in DN has not been thoroughly investigated. Therefore, we performed a retrospective cohort study to examine whether O3FA supplementation could preserve renal function in diabetic subjects.
Materials and Methods
In this retrospective study, subjects were identified by reviewing patient case notes using electronic medical records at Severance Hospital, a tertiary university hospital in Korea. We included 344 patients ≥ 20 years old with a history of O3FA (highly purified ethyl ester concentrate of EPA and DHA) supplementation for managing hypertriglyceridemia. Diabetes mellitus (DM) was defined according to the International Classification of Diseases 10th revision (ICD 10). Only new users who had not used O3FAs in a preceding year were enrolled. The mean supplement duration (‘after treatment’ period) was 1.9 ± 1.6 years (median 1.4 years). O3FA was used for at least 3 months. Subjects were excluded if they fulfilled any one of the following criteria: (1) kidney transplanted patient; (2) dialysis patient; (3) intrinsic renal disease (nephritis or nephrotic syndrome) patient; (4) acute renal failure due to septic shock, contrast agents, or drugs; and (5) postrenal disease patient. The patient records was anonymized and de-identified prior to analysis. The study protocol received ethical approval by the institutional review board at the Yonsei University College of Medicine (4-2014-0273).
Clinical and laboratory parameters
We evaluated the effects of O3FAs on DN and albuminuria. The dose-effect relationships between O3FAs and albuminuria, renal function were also analyzed. Baseline estimated glomerular filtration rates (GFRs), and spot urine ACRs were measured at the start of O3FA administration. Overnight 8-hours fasting random spot urine samples were collected, and urine ACR was measured with an immunoturbidimetric method. After O3FA treatment (median 1.4 years), we evaluated changes in these laboratory parameters and also examined clinical parameters, blood glucose, lipid profiles. GFR was calculated using the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) equation [19]. Body mass index (BMI) was defined as body weight (kg) divided by the square of height (m2).
Data analysis
The primary outcome was renal function changes during O3FAs supplementation, specifically in GFR and urine ACR. We compared the annual rates of GFR decline among three dose categories: 1 g/day, 2 g/day, and 4 g/day. Subgroup analyses were stratified according to daily O3FA doses; daily doses of 4 g O3FA were grouped into the high-dose group, and those <4 g were placed in the low-dose group. In addition, the proportion of subjects with preserved GFR was analyzed according to O3FA dosages.
Statistical analysis
The data are reported as mean ± standard deviation (SD), and the real numbers of participants with the percentages follow in parentheses. Simple comparisons of continuous variables within or between sub-groups were made with Student’s t-tests. Paired data measured at baseline and after O3FA supplementation were compared using paired t tests. Since urine ACR, total cholesterol, triglyceride, high density lipoprotein (HDL) cholesterol, and high sensitivity C-reactive protein (hsCRP) values were not normally distributed, analyses were performed using log- and back-transformed data. Chi-square tests were used to examine the relationships between multiple variables. The relative factor for GFR decline was obtained using univariate and multiple logistic regressions, and the risk is reported in the form of odds ratios (ORs) and 95% confidence intervals (CIs). All statistical analyses were performed using the SPSS statistical analysis program (SPSS vs. 20.0, IBM Corp, Armonk, NY). For all tests, p < 0.05 was considered statistically significant.
Results
Subject clinical characteristics
Table 1 shows the baseline clinical characteristics of patients. A total of 344 patients (244 males, 100 females) were recruited with a mean O3FA supplement duration of 1.9 ± 1.6 years. More than 90% of patients were treated with O3FA < 4 g/day. Three-quarters of patients had hypertension that was relatively well-controlled (mean systolic blood pressure 127.8 ± 15.1 mmHg, mean diastolic blood pressure 74.9 ± 9.6 mmHg). About 72% of these patients were using angiotensin converting enzyme (ACE) inhibitors or angiotensin receptor blockers (ARBs).
Effects of O3FA supplementation on renal function loss
Urine ACR was significantly decreased after O3FA supplementation (from 475.8 ± 1235.9 mg/g to 385.6 ± 1067.9 mg/g, Δ = -72.1 ± 507.6 mg/g, p = 0.003; Table 2). However, a significant GFR decline was observed during the study periods (Table 2). The mean annual GFR loss was 2.6 ± 12.7 mL/min/1.73 m2 (median value 0.9 mL/min/1.73 m2). GFR did not decrease in 172 (50.0%) patients and increased in 125 (36.3%) patients after O3FA supplementation. We also analyzed the baseline characteristics of study groups stratified by whether GFR was preserved (S1 Table). There were no significant differences in baseline parameters according to the presence of GFR loss in renal function, except for diabetes duration, O3FAs dose, systolic blood pressure, and urine ACR. The shorter diabetes duration and lower urine ACR the patients had, the greater the benefit to preserving GFR was observed (S1 Table). Greater maintenance of renal function was observed in the high dose group (Table 3). The annual decline in GFR ranged from 3.6 ± 10.8 mL/min/1.73 m2 in the 1 g/day group to 2.6 ± 13.7 mL/min/1.73 m2 in the 2 g/day group. For the 4 g/day group, the GFR decline was -0.3 ± 11.5 mL/min/1.73 m2. However, there was no statistically significant difference in annual GFR loss among these three groups. The proportions of patients without GFR decline were 37.9%, 54.0%, and 63.3% in the 1 g/day, 2 g/day and 4 g/day groups, respectively (p = 0.006 for trend). Univariate logistic regression analysis was performed to identify variables associated with kidney function loss (Table 3). In terms of GFR loss, O3FA doses of 2 g/day (OR = 0.52, 95% CI 0.32–0.84, p = 0.008) and 4 g/day (OR = 0.35, 95% CI 0.15–0.82, p = 0.015) were beneficial, whereas longer diabetes duration, higher systolic blood pressure, and fenofibrate use had a negative effect (Table 3). Next, we sought to confirm the efficacy of high-dose O3FAs on DN. As shown in S2 Table, patients treated with high doses of O3FAs tended to have increased baseline triglycerides and fenofibrate use. Multivariable logistic regression models were applied to adjust for other conventional confounding covariates that affect DN, along with fenofibrate, statin use, and triglycerides levels (Table 4). O3FA at 2 g/day had a positive effect on GFR preservation (OR = 0.43, 95% CI 0.26–0.74, p <0.05), on which O3FA at 4 g/day showed a markedly higher benefit (OR = 0.20, 95% CI 0.08–0.52, p <0.05). The same trends were observed in patients without fenofibrate use (S3 Table).
Effects of O3FA supplementations on metabolic parameters
At enrollment, 61.3% of patients were using statins, and 15.7% used fenofibrate. Serum triglyceride levels were 46% lower after O3FA supplementation (p < 0.001), and total cholesterol decreased by 19% (p < 0.001). There were no significant changes in HDL cholesterol after O3FA treatment (Table 2). However, uric acid levels and hsCRP were significantly reduced (All ps < 0.05, Table 2).
Discussion
The major finding of this study is that O3FA supplementation may help with preserving renal function in type 2 diabetes patients with hypertriglyceridemia. O3FA influenced both urine ACR and GFR, indicating a protective effect for O3FA on DN. In addition, the effects were dependent on the dose of daily O3FA supplementation. Although GFR decline was observed in our study population, the mean annual rate of GFR decline was relatively slower than that reported in a previous study [5].
A possible association between O3FA supplementation and albuminuria reduction was first noticed after EPA was found to improve albuminuria in diabetic patients [20]. After EPA was administered to 16 diabetic patients (5 type 1 and 11 type 2) for 6 months, albuminuria measured with spot urine was significantly improved without altering blood glucose levels, body weight, or blood pressure. A large nested control study including 1,150 type 1 DM subjects showed that higher n-3 PUFA intake was related to a lower risk of microalbuminuria [21]. There are also some studies supporting the hypothesis that O3FA supplementation slows the progression of IgA nephropathy. For IgA nephropathy patients with persistent proteinuria, fish oil supplementation for 2 years delayed nephropathy progression compared to olive oil supplementation, and this effect appeared to be independent of reduced blood pressure [16]. A meta-analysis showed n-3 PUFA reduces urine protein excretion among IgA nephropathy, DM, and lupus nephritis patient populations [22]. In addition, O3FA supplementation reportedly reduces DM complications [23]. The pathway of beneficial effects of O3FA in kidney has been studied in animal experiments: improvement of dyslipidemia and attenuation of inflammation. Streptozotocin-induced diabetic rats fed a high n-3 PUFA diet were more resistant to renal disease development [24]. N-3 PUFA treatment attenuated diabetes-associated glomerulosclerosis and tubulointerstitial fibrosis [24]. In addition, after n-3 PUFA supplementation, expression levels of transforming growth factor (TGF)-β, which is a marker of end-organ complications associated with DM, and those of interleukin (IL)-6 and monocyte chemoattractant protein (MCP)-1, markers of tissue inflammation, were attenuated [24]. Similarly, in DN of type 2 diabetic KKAy/Ta mice model, improved urine ACR and down regulated MCP-1 levels were observed [25]. Mesangial matrix accumulation and tubule-interstitial fibrosis were attenuated in EPA-injected mice, but where were no alterations in systolic blood pressure or fasting blood glucose levels [25]. Moreover, O3FA fed db/db mice showed reductions in renal triglycerides and renal SREBP-1 expression, as well as attenuation of podocyte injury [26]. In our study, although levels were only measured in half of the patients hsCRP levels were significantly reduced after O3FAs supplementation.
The dose-related effect of O3FAs on DN has not been studied, but it has been investigated in the context of heart disease. According to the American Heart Association guideline, consuming 2 servings (8 ounces) of food containing very long-chain O3FAs reduces the risks of sudden death and death from coronary artery disease [27]. The mechanisms by which O3FAs influence cardiovascular disease include amelioration of arrhythmias, thrombosis, inflammatory responses, triglycerides, remnant lipoprotein levels, low-density lipoprotein cholesterol, atherosclerotic plaque instability, endothelial dysfunction, and blood pressure [28, 29]. Among these factors, lowered triglyceride efficacy is thought to be a dose-response effect of O3FAs [30]. In previous studies, 4 g/day of O3FAs reduced serum triglyceride levels by up to 30% [31–34]. A comparison study of O3FAs dose-response effects on triglycerides in healthy individuals demonstrated that high-dose (3.4 g/day) O3FAs significantly decreased triglyceride, whereas there were no changes in blood triglyceride levels in the placebo or low-dose (0.85 g/day) groups [35].
Studies suggest that statin could reduce albuminuria and slow down kidney function loss [36–38]. In subgroup analysis of the Greek atorvastatin and coronary heart disease evaluation study (GRACE), creatinine clearance increased in patients with statin use (4.9%, p = 0.003) [36]. Interestingly, among statin users, patients treated with atorvastatin experienced better renal outcomes, with a 12% increase in creatinine clearance (p <0.001) [36]. The renoprotective effect of statin is based on the fact that dyslipidemia and hypertension accelerate renal function loss [38]. In our study, 78 subjects were prescribed atorvastatin (37.0%) among patients treated with any statin. The proportions of those with preserved GFR were 51.1% for non-statin users and 49.3% for stain users (p = 0.740). In addition, 48.7% of atorvastatin (median dose 10 mg/day) users showed preserved GFR, which was similar to that for other statin users (49.6%) (p = 0.899). The median dose of atorvastatin in our study was 10 mg/day, which was lower than that in a previous study (24 mg/day) [36]. As the lipid lowering effect of atorvastatin depends on the daily dose [37], the difference in atorvastatin dose would lead to discordant results. Meanwhile, the association between fenofibrate, another lipid lowering drug, and renoprotective effect is controversial [39–42]. It might reduce albuminuria by antioxidant and anti-inflammatory mechanisms, in addition to a hypertriglyceridemia lowering effect [39, 40]. In an international study on type 2 diabetes patients, a fenofibrate treatment group experienced 2.6% regression or no progression in renal function deterioration, compared to a placebo group (p = 0.002) [41]. Moreover, 5-year use of fenofibrate was found to reduce albuminuria and inhibit GFR decline independently from ACE inhibitor/ARB use [39]. However, others have reported decreases in creatinine clearance and GFR with fenofibrate use [42]. In our study, as shown in univariate analysis (Table 3), fenofibrate use showed a negative effect on preserving renal function. We then conducted subgroup analysis excluding subjects with fenofibrate use. Therein, as shown in S3 Table, O3FA supplement was still associated with maintaining kidney function in a dose dependent manner.
Conversely, there are some reports that O3FA supplementation is not associated with reduced albuminuria or that this effect is not dose-dependent. A cohort study assessed both type 1 and 2 DM patients with microalbuminuria and reported that treatment with 4 g/day of O3FAs did not improve albuminuria [43]. However, the study enrolled a small number of patients, and the total treatment duration was only 12 weeks. A randomized trial assessing severe IgA nephropathy patients showed no additional benefit of high-dose O3FA supplementation [44]. In our data, O3FAs reduced urine ACR or preserved GFR was mostly observed in patients with early DN. This might explain why O3FAs did not have dose-dependent effects in patients with severe IgA nephropathy. In a randomized trial with type 2 diabetes patients, 4 g/day of n-3 PUFA supplement during 6 weeks did not show significant changes in urine ACR [45]. However, there was significant improvement in serum renal damage markers, suggesting the beneficial effect of n-3 PUFA on renal function.
Our study had several limitations. Because it was a retrospective investigation, there were many critical confounders influencing albuminuria or nephropathy. First, ACE inhibitors and ARBs are known to ameliorate albuminuria in DN. More than half of patients (71.8%) were prescribed those medications. Although there were no differences in medication use between the GFR decline progression and no-progression groups, we analyzed ACE inhibitor or ARB use as a covariate factor. Second, medication compliance was not fully considered. As this was not a prospective study, we could not assess adherence with the prescribed O3FA. The study data were based on the proposition that all the prescribed medication was administrated to the subjects. Third, hyperglycemia was improved in the course of the study. Fasting and postprandial blood glucose levels were significantly decreased after O3FAs supplementation. There is a possibility that improved hyperglycemia may contribute to renal function maintain. However, the correlation analysis showed that improvement in serum triglyceride level is more closely associated with better GFR maintain after adjustment fasting blood glucose reduction (r = 0.18, p = 0.001). Fourth, most patients enrolled in this study were relatively early stage DN, as 77.9% of patients were treated with metformin (contraindicated for advanced kidney disease patients) and > 70% of patients were normo-, or microalbuminuria or CKD stage I or, II. In addition, we did not include a control group. However, it would be immoral practice to prescribe a placebo to patients with hypertriglyceridemia, especially to subjects with serum triglyceride more than 500 mg/dl, due to the risk of acute pancreatitis.
Our study also had a major strength. We showed dose dependency in O3FAs effects on attenuating GFR loss. This is the first study reporting an association between O3FA supplementation dosages and DN. A novel finding is the identification of an effective O3FA dose in DN patients with hypertriglyceridemia. In addition, we enrolled compliant patients without other kidney diseases who were selected based on detailed reviews of their medical records.
In conclusion, our findings demonstrate that O3FA supplementation in diabetic patients with hypertriglyceridemia ameliorated urine ACR and preserved GFR. This suggests that O3FA supplementation in diabetic patients with hypertriglyceridemia could ameliorate DN progression in a dose-dependent manner. However, further randomized trials are needed to quantify this beneficial effect compared to placebo and control groups. If there is clear dose-dependent effect of O3FAs on DN, high-dose O3FA administration will likely provide a therapeutic option for high-risk diabetic patients.
Supporting Information
S1 Dataset. The anthropometric and biochemistry characteristics of the subjects.
https://doi.org/10.1371/journal.pone.0154683.s001
(XLSX)
S1 Table. Baseline characteristics of patients preserved GFR.
Data are presented as N(%) or mean ± SD. DM, diabetes mellitus; O3FAs, omega-3 fatty acid; BMI, body mass index; ACEi, angiotensin-converting enzyme inhibitor; ARB, angiotensin II receptor blocker; CCB, calcium channel blocker; SU, sulfonylurea; DPP4i, dipeptidyl peptidase-4 inhibitor; TZD, thiazolidinedione; Urine ACR, urine albumin to creatinine ratio; GFR, glomerular filtration rate; HbA1c, glycated hemoglobin; HDL cholesterol, high-density lipoprotein cholesterol; hsCRP, high sensitivity c-reactive protein.*Log transformed.
https://doi.org/10.1371/journal.pone.0154683.s002
(DOCX)
S2 Table. Baseline characteristics of patients according to O3FAs daily dose.
Data are presented as N(%) or mean ± SD. BMI, body mass index; HDL cholesterol, high density lipoprotein cholesterol; GFR, glomerular filtration rate; ACR, albumin to creatinine ratio; ACE inhibitor, angiotensin-converting enzyme inhibitor; ARB, angiotensin II receptor blocker.*Log transformed.
https://doi.org/10.1371/journal.pone.0154683.s003
(DOCX)
S3 Table. Multiple logistic regression analysis to determine variables associated GFR decline in subjects without fenofibrate use.
Reference group = patients with O3FA 1g/day, Model 1: adjusted for age and sex, Model 2: adjusted for age, sex, diabetes duration, body mass index, systolic blood pressure, angiotensin-converting enzyme inhibitor/angiotensin II receptor, and statin use, Model 3: adjusted for age, sex, diabetes duration, body mass index, systolic blood pressure, angiotensin-converting enzyme inhibitor/angiotensin II receptor, statin, fenofibrate, fasting blood glucose, baseline GFR, triglycerides, and total cholesterol. GFR, glomerular filtration rate; O3FAs, omega-3 fatty acids; OR, odds ratio; 95% CI, 95% confidence interval.
https://doi.org/10.1371/journal.pone.0154683.s004
(DOCX)
Acknowledgments
The authors thank the study participants for their contribution to the research. All authors state that they have no conflicts of interest and no competing financial interests.
Author Contributions
Conceived and designed the experiments: EH YY ESK. Performed the experiments: EH YY ESK. Analyzed the data: EH YY GK YL HJW. Contributed reagents/materials/analysis tools: BWL BSC BSK ESK. Wrote the paper: EH YY ESK.
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