Serum Levels of Adipocyte Fatty Acid-Binding Protein Are Associated with Rapid Renal Function Decline in Patients with Type 2 Diabetes Mellitus and Preserved Renal Function
Article information
Abstract
Background
Recent studies have demonstrated that the levels of adipocyte fatty acid-binding protein (A-FABP) are closely associated with diabetic kidney disease (DKD) in patients with type 2 diabetes mellitus (T2DM). This study aimed to examine the association between serum A-FABP level and rapid renal function decline in patients with T2DM and preserved renal function.
Methods
This was a prospective observational study of 452 patients with T2DM and preserved renal function who had serial measurements of estimated glomerular filtration rate (eGFR). Rapid renal function decline was defined as an eGFR decline of >4% per year. The association between baseline serum A-FABP level and rapid renal function decline was investigated.
Results
Over a median follow-up of 7 years, 82 participants (18.1%) experienced rapid renal function decline. Median A-FABP levels were significantly higher in patients with rapid renal function decline, compared to non-decliners (20.2 ng/mL vs. 17.2 ng/mL, P=0.005). A higher baseline level of A-FABP was associated with a greater risk of developing rapid renal function decline, independent of age, sex, duration of diabetes, body mass index, systolic blood pressure, history of cardiovascular disease, baseline eGFR, urine albumin creatinine ratio, total cholesterol, glycosylated hemoglobin, high-sensitivity C-reactive protein and use of thiazolidinedione, insulin, angiotensin-converting-enzyme inhibitors and angiotensin II-receptor blockers and statin (odds ratio, 3.10; 95% confidence interval, 1.53 to 6.29; P=0.002).
Conclusion
A high level of serum A-FABP is associated with an increased risk of rapid renal function decline in patients with T2DM and preserved renal function. This suggests that A-FABP could play a role in the progression of DKD in the early stages.
INTRODUCTION
The prevalence of diabetic kidney disease (DKD) continues to increase worldwide, leading to rising morbidity and premature mortality in patients with diabetes [1]. Despite significant advances in identifying new mechanisms for DKD over the years, factors contributing to the natural course or progression of DKD in people with type 2 diabetes mellitus (T2DM) have remained unclear. DKD has been traditionally characterized by albuminuria, followed by reduced glomerular filtration rate (GFR) [2]. However, recent studies on T2DM have shown that subjects can also develop non-albuminuric renal insufficiency, suggesting that albuminuria is not a prerequisite for the development of DKD [34].
The Joslin Kidney Study in patients with type 1 diabetes mellitus explored the trajectories of estimated glomerular filtration rate (eGFR) decline over the years and found that most patients had a linear eGFR decline. There was a subset of patients who developed early rapid renal function decline, which occurred when they had normal renal function, and the decline in eGFR continued until they reached end stage renal disease (ESRD) [5]. It was suggested that rapid renal function decline is another strong predictor of progression to ESRD [56]. Similarly, studies in patients with T2DM also showed that most patients have a linear eGFR decline starting at an early stage and the slope varies substantially among patients [478]. Similarly, patients with T2DM also had a subgroup of patients who had steeper renal function decline [9], which predicted ESRD and premature mortality [10]; however, the definitions of rapid decline were not uniform among these studies [611]. Clinical factors associated with rapid renal function decline in patients with T2DM have been explored in several studies, but the findings were inconsistent [12].
Adipocyte fatty acid-binding protein (A-FABP) is an adipokine that is preferentially expressed in adipocytes [13]. Recent studies in animal models have demonstrated that circulating A-FABP is associated with glucose homeostasis via direct induction of insulin resistance [14]. Moreover, several human studies have demonstrated that serum A-FABP levels predict the development of metabolic syndrome, T2DM, carotid atherosclerosis, and nonalcoholic fatty liver disease [151617]. Cross-sectional studies in patients with T2DM have suggested that an association exists between serum A-FABP levels and DKD. Serum A-FABP levels were reported to have a negative correlation with eGFR but a positive correlation with microalbuminuria [181920]. Furthermore, a recent prospective study in patients with T2DM demonstrated that higher levels of A-FABP independently predicted adverse renal outcomes [21]. However, to our knowledge, the role of the level of circulating A-FABP in significant renal function decline in patients with T2DM and preserved renal function has not yet been elucidated. Therefore, we performed this prospective study to evaluate whether baseline serum A-FABP levels were independently associated with the development of rapid renal function decline in patients with T2DM and preserved renal function. Other relevant adipokines and cytokines, including pentraxin-3 (PTX3), were also examined.
METHODS
Study population
The study population consisted of 452 subjects with T2DM and preserved renal function, defined by eGFR ≥60 mL/min/1.72 m2. The patients were recruited from the outpatient clinic of the Diabetes Center of Inha University Hospital in Incheon, Korea from March 2007 to December 2009. The inclusion criteria were; patients older than 20 years of age, diagnosed with T2DM based on the American Diabetes Association criteria [22], and/or being treated with oral hypoglycemic agents or insulin or lifestyle modification for known T2DM. The exclusion criteria were: patients with congestive heart failure, severe infection, uncontrolled hypertension, severe dyslipidemia (total cholesterol >400 mg/dL), a medical condition requiring active management, diabetes duration <1 year, or an eGFR <60 mL/min/ 1.73 m2 and <4 annual GFR measurements during the follow-up. The study protocol was approved by the Institutional Review Board of Inha University Hospital, and all participants provided written informed consent prior to participation (IRB No., 2006-67).
Demographic, physical, and laboratory measurements
During interviews, trained personnel obtained medical history information from all patients. Height and weight were measured to the nearest 0.1 cm and 0.1 kg, respectively. Body mass index (BMI) was defined as weight (kg) divided by height (m) squared. Waist circumference was measured at the midpoint between the lower borders of the rib cage and the iliac crest. Blood pressure (BP) was measured after the subject had rested for at least 10 minutes in a sitting position. Diabetic retinopathy was diagnosed based on funduscopic examinations. Hypertension was defined as BP ≥140/90 mm Hg or treatment with any antihypertensive drug. Cardiovascular disease (CVD) was defined as the presence of ischemic heart disease, including stable angina, acute coronary syndrome, and myocardial infarction with ST-segment elevation.
Blood samples were collected after an overnight fast of at least 10 hours and stored at −70℃ until subsequent assays. Laboratory measurements, including fasting serum glucose, lipid subfractions, glycosylated hemoglobin (HbA1c), and 75 g oral glucose tolerance testing were conducted in a fasted state. The level of high-sensitivity C-reactive protein (hs-CRP) was measured using a particle-enhanced immunoturbidimetric assay (Hitachi High-Technologies Corp., Tokyo, Japan). Homeostasis model assessment of insulin resistance (HOMA-IR) levels were calculated by dividing the product of insulin (microunits per milliliter) and glucose (millimoles per liter) concentrations by 22.5 [23]. A random urine sample was obtained for albumin creatinine ratio (ACR) measurements. Albuminuria was classified into three stages: normoalbuminuria was defined as spot urine ACR (UACR) <30 µg/mg Cr, microalbuminuria as UACR ≥30 µg/mg Cr and <299 µg/mg Cr, and macroalbuminuria as UACR ≥300 µg/mg Cr [24].
Renal function measurement
The eGFR values were calculated using the Chronic Kidney Disease Epidemiology Collaboration (CKD-EPI) creatinine equation [25], as follows: eGFR=141×min (Scr/κ, 1)α×max (Scr/κ, 1)−1.209×0.993Age×1.018 (if female); where, Scr is serum creatinine in mg/dL, κ is 0.7 for females and 0.9 for males, α is −0.329 for females and −0.411 for males, min is the minimum value of Scr/κ or 1, and max is the maximum value of Scr/κ or 1. Annual eGFR decline was calculated as follows; for each patient, a linear regression model of time on eGFR (least-squares method) was fitted, and the slope of the regression line was used to estimate the changes in patient's eGFR over time. The eGFR slope was expressed as a percentage per year by dividing the slope with the baseline eGFR value [11]. Rapid renal function decline was defined as eGFR decline >4% per year, in accordance with previous studies [11]; this threshold represents an eGFR loss ≥3 mL/min/1.73 m2 per year, which is the cutoff value for representing a magnitude of change that is three times the rate of normal aging [26].
Measurement of cytokine levels
Enzyme-linked immunosorbent assays (ELISAs) were used to measure the serum concentration of A-FABP (Biovendor Laboratory Medicine, Modrice, Czech Republic), total adiponectin and high molecular weight (HMW) adiponectin (ALPCO Diagnostics, Salem, NH, USA), tumor necrosis factor-α (TNF-α), interleukin 6 (IL-6), and PTX3 (R&D Systems, Minneapolis, MN, USA). The intra- and inter-assay coefficients of variation (%) were 2.5% and 6.1% for A-FABP, 5.3% and 5.0% for total adiponectin, 3.3% and 5.7% for HMW adiponectin, 3.1% and 7.4% for TNF-α, 6.9% and 6.5% for IL-6, and 7.3% and 3.4% for PTX3.
Statistical analysis
Data are presented as the mean±standard deviation, median (interquartile range [IQR]), or as numbers (percentages). Baseline characteristics of the participants were compared using Student's t test or Wilcoxon rank-sum test for continuous variables and Pearson's chi-square test for categorical variables, as appropriate. Correlations between annual renal function decline (%) and serum levels of various cytokines or adipokines after adjustment for age, sex, BMI, HbA1c, and baseline eGFR were analyzed using the partial Spearman correlation analysis. To evaluate the difference in clinical characteristics based on the A-FABP tertiles, the cutoff level for each tertile was calculated separately for men and women because A-FABP levels differ significantly by sex. P for trend was calculated using a contrast to test for linear trends in continuous variables and the Cochran-Armitage test for categorical variables.
Multivariable logistic regression models were built to test our hypothesis that high serum A-FABP level at baseline might be an independent risk factor for rapid renal function decline. The fully adjusted model included clinical risk factors, such as age, sex, duration of diabetes, BMI, systolic blood pressure (SBP), history of cardiovascular disease, baseline eGFR, UACR, total cholesterol, HbA1c, hs-CRP and use of thiazolidinedione, insulin, angiotensin-converting-enzyme inhibitors and angiotensin II-receptor blockers and statin. All analyses were done with 95% confidence interval (CI), and the level of significance was determined at P<0.05. Statistical analysis was performed with SPSS version 19.0 statistical package software (IBM Corp., Armonk, NY, USA).
RESULTS
Baseline characteristics of study participants
The mean age of the participants was 52.6±9.2 years, 69.2% of them were men, mean duration of diabetes was 5.6±5.1 years, mean HbA1c was 7.9%±1.7%, and baseline eGFR was 85.8±14.9 mL/min/1.73 m2. Of all the participants, 314 (69.5%) had normoalbuminuria, 114 (25.2%) had microalbuminuria, and 11 (2.4%) had macroalbuminuria. In total, 181 (40.0%) participants had hypertension and 17 (3.8%) had previous history of CVD. During a median follow-up of 7 years (range, 3 to 9 years), all the patients had at least four annual measurements of eGFR. Median annual eGFR decline (%) of the whole cohort was −2.0% per year. During the follow-up period, 82 patients (18.1%) developed rapid renal function decline (rapid decliners). Median annual eGFR decline (%) was −5.8% per year in rapid decliners and −0.9% per year in non-decliners (P<0.001). Three patients developed ESRD at the end of the follow-up.
Baseline characteristics of rapid decliners (n=82) and non-decliners (n=370) are summarized in Table 1. Rapid decliners were significantly older and had higher levels of baseline eGFR and total cholesterol. No difference was noted in UACR at baseline between the groups. The majority of the rapid decliners had normoalbuminuria at baseline (75.6%), which was comparable with that of the non-decliners (70.6%).
Levels of serum A-FABP and other cytokines according to the presence of rapid renal function decline
Baseline median serum A-FABP levels were significantly higher in rapid decliners compared to non-decliners (20.2 µg/L vs. 17.2 µg/L, P=0.005) (Table 1, Fig. 1B). When stratified for sex, similar findings were noted for both men and women (Table 1). Serum A-FABP levels were significantly higher in women than in men (23.1 µg/L vs. 15.8 µg/L, P<0.001) (Fig. 1A). Consistent with previous reports [1213], patients with micro or macroalbuminuria had significantly higher median serum A-FABP concentrations than those with normoalbuminuria (19.5 µg/L vs. 16.6 µg/L, P=0.042) (Fig. 1C). Median serum levels of total adiponectin, HMW, IL-6, TNF-α, and PTX3 showed no difference between rapid decliners and non-decliners.
Correlation between annual renal decline (%) and serum level of A-FABP and other adipocytokines
As shown in Table 2, partial Spearman's correlation analyses was performed to investigate the correlations between annual renal function decline (%) and serum levels of adipokines or cytokines after adjusting for clinical risk factors, including age, sex, BMI, HbA1c, and baseline eGFR. Serum A-FABP showed a negative correlation with annual renal function decline (%) (r=−0.150, P=0.005). No significant correlation was observed between annual renal function decline (%) and other adipokines or cytokines.
Independent association between serum A-FABP level and rapid renal function decline
To assess the characteristics of the patients according to the A-FABP levels, the participants were subgrouped into tertiles based on serum A-FABP levels. The incidence of rapid renal function decline in the lowest (T1) to highest (T3) A-FABP tertiles was 12.7%, 16.6%, and 25.2%, respectively (Ptrend 0.016) (Table 3). Participants in the higher tertiles were older, had a longer duration of diabetes, lower baseline eGFR, and faster eGFR decline per year (%), but no differences were found in baseline UACR. However, the A-FABP level was not significantly associated with other inflammatory markers. Multivariable logistic regression analysis showed that baseline serum A-FABP level was independently associated with a greater risk of rapid renal function decline (Model 1; odds ratio [OR] , 1.81; 95% CI, 1.17 to 2.80) after adjustment for age (Table 4). This association remained significant after further adjustment for other factors, including sex, duration of diabetes, BMI, SBP, history of cardiovascular disease, baseline eGFR, UACR, total cholesterol, glycosylated hemoglobin, hs-CRP and use of thiazolidinedione, insulin, angiotensin-converting-enzyme inhibitors and angiotensin II-receptor blockers and statin (OR, 3.10; 95% CI, 1.53 to 6.29; P=0.002). When the analysis was stratified by sex, this association remained robust in both men and women (OR, 2.65; 95% CI, 1.10 to 6.38 and OR, 5.65; 95% CI, 1.17 to 27.19 for males and females, respectively) (Table 4).
DISCUSSION
In this prospective study of patients with T2DM and preserved renal function, we demonstrated that the baseline serum A-FABP level was independently associated with the development of early rapid renal function decline during 7 years of follow-up. Higher baseline serum A-FABP level was associated with a greater risk of developing rapid renal function decline in patients with T2DM and preserved renal function, independent of other clinical risk factors.
A few studies have demonstrated that there is an independent association between A-FABP and diabetic nephropathy [181920]. However, most of these published studies are limited by small sample sizes and cross-sectional settings. A prospective study by the Hong Kong West Diabetes Registry was published while our manuscript was in preparation and showed that the level of circulating A-FABP was independently associated with the development of adverse renal outcomes in patients with T2DM, suggesting a significant role of serum A-FABP in DKD as seen in our study [21]. In the present study, we found that a higher baseline serum A-FABP level was independently associated with the development of early rapid renal function decline in individuals with T2DM and preserved renal function. As filtration through the kidneys is an important route of A-FABP clearance [27], we exclusively enrolled individuals with preserved renal function whereas other studies had also included participants with impaired renal function. Consistent with the results of previous studies on rapid renal function decline in patients with T2DM [711], the overall incidence of rapid renal function decline in the current study was 18.1% during the median follow-up of 7 years. Patients in the highest and lowest A-FABP tertiles had incidence rates of 25.2% and 16.6%, respectively.
Serum A-FABP levels were significantly higher in females than in males as previously reported [1628]. Although the reason for this difference is not clearly understood it has been speculated that sex hormones, especially androgen, play critical roles in the production and distribution of body fat [29], which regulates circulating A-FABP levels [30]. When analysis was done separately for males and females, serum levels of circulating A-FABP remained independently associated with rapid renal function decline in both males and females.
Although the exact mechanisms underlying rapid renal function decline are unknown, our findings may implicate the potential role of A-FABP in the development and progression of DKD, especially in the early stages. While the Hong Kong study examined the association between baseline serum A-FABP level and hard renal outcomes such as a sustained 40% decline in eGFR, ESRD requiring renal replacement therapy or kidney transplantation, or death from renal causes [21], the primary endpoint in the present study was early rapid renal function decline, an outcome that can more sensitively identify patients that are at high risk during the early stages. Early rapid renal function decline is considered a unidirectional process that occurs while patients have normal kidney function and steadily progresses to ESRD [5]; yet, there is no effective prognostic tool or marker that identifies rapid decliners in clinical settings. While both albuminuria and reduced eGFR are independent risk factors of ESRD [31], they are of little value to distinguish non-decliners from rapid decliners during the early stages. Conversely, this study demonstrated the potential implication of serum A-FABP as a clinical marker for identifying rapid decliners among patients with T2DM and normal kidney function. It is particularly relevant, as, at present, a good prognostic test to identify rapid decliners while they have normal renal function is not available. Furthermore, there is emerging evidence suggesting an increase in the prevalence of DKD without accompanying albuminuria [3], and our study demonstrated that baseline serum A-FABP was significantly associated with rapid renal function decline even after adjustment for baseline UACR. Collectively, these findings provide further evidence for the potential role of A-FABP in the pathogenesis of DKD during the earlier stages when no clinical manifestation is present.
Although the exact role of A-FABP in the pathogenesis of rapid renal function decline is not fully understood and is beyond the scope of the current study, there may be a few possible mechanisms. Previous animal studies on A-FABP−/− mice showed that they were protected from the development of obesity-induced insulin resistance and diet-induced atherosclerosis [32], and mice treated with an A-FABP inhibitor demonstrated improvement in metabolic profiles as well as marked reduction in atherosclerotic lesions [33]. Similar findings were also noted in humans; where, increased A-FABP synthesis in atherosclerotic plaques was associated with disease severity [32]. As atherosclerosis plays a critical role in the development of early DKD [34], A-FABP may promote atherosclerotic disease, which, in turn, can lead to rapid renal function decline in patients with T2DM. These findings are further supported by our recent study in patients with T2DM and preserved renal function; where, there was a strong association between carotid atherosclerosis and rapid renal function decline [35].
Secondly, increased levels of A-FABP may be an indicator of the abnormal angiogenesis that is involved in the pathogenesis of the early stages of DKD. A-FABP has been primarily regarded as an adipocyte and macrophage-specific intracellular lipid-binding protein [36]. However, recent studies have demonstrated that A-FABP is also expressed in microvascular endothelial cells, including peritubular capillaries of the kidney, in an angiogenesis-dependent manner in both mice and humans [36]. Previous studies on DKD indicated that abnormal angiogenesis is involved in the development of diabetic nephropathy, which is triggered by high glucose levels as well as glomerular hypertension [37]. Additionally, upregulation of vascular endothelial growth factor expression was also observed, which acts as a mediator of abnormal angiogenesis in diabetic nephropathy as well as a regulator of A-FABP in endothelial cells [3637]. Thus, an elevated serum A-FABP level at baseline may indicate the increased expression of A-FABP in the renal tubules as well as endothelial cells of tubular capillaries, suggesting that abnormal angiogenesis and accumulation of macrophages and proinflammatory cytokines occur in the kidneys prior to the impairment of renal function. Accordingly, measuring serum A-FABP levels may offer additive information to identify the patients at risk of developing early DKD.
Increasing evidence also points to the critical roles of proinflammatory cytokines in the development and progression of DKD. Longitudinal studies have shown a positive relationship between hs-CRP, TNF-α, IL-6, and progression of DKD, which is often correlated with albuminuria [3839]. Another study also demonstrated that both serum and urinary TNF-α levels were increased in diabetic patients with albuminuria, but no correlation was found in patients with normoalbuminuria [40]. Urine concentrations of cytokines, such as IL-6, were reported to be markedly elevated in rapid renal function decliners with albuminuria [5]. However, in the present study, no significant association was observed between baseline levels of inflammatory cytokines and rapid renal function decline; this may be due to differences in the study population, study endpoints, and ethnicity. In fact, the majority of the subjects in our study had normoalbuminuria at baseline (69.5%) and the proportion of subjects with normoalbuminuria was similar between rapid decliners and non-decliners. Regarding PTX3, a vascular inflammatory marker, inconsistent results have been observed in patients with DKD [41]. In our study, no association was found between PTX3 levels and rapid renal function decline.
The strength of this study includes the prospective design with serial measurements of kidney function to accurately estimate the annual eGFR decline and examine the association between rapid renal function decline and adipokines. We also confined the subjects to those with preserved renal function to assess the association between baseline serum A-FABP levels and early progressive renal disease. Moreover, our cohort consists of a large number of participants from a homogeneous population and the follow-up period was 7 years. We also measured other proinflammatory cytokines and adipokines along with serum A-FABP. To our knowledge, this is the first prospective study showing that high A-FABP serum levels at baseline are associated with increased risk of rapid renal function decline in Asian patients with T2DM and preserved renal function.
The present study, however, has some limitations. First, because our cohort comprised Korean patients with T2DM who were followed at a single, tertiary-level hospital, our results may not be directly applicable to the general population. Second, there was no direct measurement of GFR but we employed CKD-EPI equations, which have been widely used by many studies. In addition, we measured serial values over time to identify the rate of decline in eGFR that was approximated using linear slopes; the use of such slopes likely smoothed out the variability in individual GFR estimates and measurements. Third, the serum A-FABP level was determined from a single-point blood sample at baseline. Serial sampling during the natural course of T2DM could help in further elucidating the role of A-FABP in the pathophysiological mechanisms of the development and progression of DKD. Lastly, renal biopsy was not performed in the majority of subjects in our study; hence, the histological diagnosis of DKD could not be confirmed.
In conclusion, higher levels of serum A-FABP are associated with increased risk of rapid renal function decline in patients with T2DM and preserved renal function. Along with its role as a metabolic risk marker, increased levels of serum A-FABP in diabetic patients may serve as a clinical marker for early progressive renal disease, which will allow early implementation of an intensive treatment in diabetic patients with normal renal function. Further studies are warranted to elucidate the role of A-FABP in the pathophysiological mechanisms involved in the development and progression of DKD.
ACKNOWLEDGMENTS
This work was supported by an Inha University Hospital Research Grant. No funding sources were involved in the study.
Notes
CONFLICTS OF INTEREST
No potential conflict of interest relevant to this article was reported.
AUTHOR CONTRIBUTIONS
Conception or design: D.H.S., S.H.K.
Acquisition, analysis, or interpretation of data: D.H.S., M.N., M.J., Y.J.S., S.H.A., S.H., S.H.K.
Drafting the work or revising: D.H.S., M.N., M.J., S.H.A., S.H., S.H.K.
Final approval of the manuscript: S.H.K.