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Urine NGAL Predicts Severity of Acute Kidney Injury After Cardiac Surgery: A Prospective Study

Michael Bennett^*, Catherine L. Dent, Qing Ma^*, Sudha Dastrala^*, Frank Grenier, Ryan Workman, Hina Syed, Salman Ali, Jonathan Barasch, and Prasad Devarajan^*

^* Nephrology & Hypertension and, Cardiology, Cincinnati Children's Hospital Medical Center, University of Cincinnati School of Medicine, Cincinnati, Ohio; Abbott Diagnostics, Abbott Park, Illinois; and Nephrology, College of Physicians and Surgeons, Columbia University, New York, New York

Correspondence: Dr. Prasad Devarajan, Nephrology & Hypertension, MLC 7022, 3333 Burnet Avenue, Cincinnati, OH 45229-3039. Phone: 513-636-4531; Fax: 513-636-7407; E-mail: prasad.devarajan{at}cchmc.org

	Abstract

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Background and objectives: The authors have previously shown that urine neutrophil gelatinase-associated lipocalin (NGAL), measured by a research ELISA, is an early predictive biomarker of acute kidney injury (AKI) after cardiopulmonary bypass (CPB). In this study, whether an NGAL immunoassay developed for a standardized clinical platform (ARCHITECT analyzer®, Abbott Diagnostics Division, Abbott Laboratories, Abbott Park, IL) can predict AKI after CPB was tested.

Design, setting, participants, & measurements: In a pilot study with 136 urine samples (NGAL range, 0.3 to 815 ng/ml) and 6 calibration standards (NGAL range, 0 to 1000 ng/ml), NGAL measurements by research ELISA and by the ARCHITECT® assay were highly correlated (r = 0.99). In a subsequent study, 196 children undergoing CPB were prospectively enrolled and serial urine NGAL measurements obtained by ARCHITECT® assay. The primary outcome was AKI, defined as a 50% increase in serum creatinine.

Results: AKI developed in 99 patients (51%), but the diagnosis using serum creatinine was delayed by 2 to 3 d after CPB. In contrast, mean urine NGAL levels increased 15-fold within 2 h and by 25-fold at 4 and 6 h after CPB. For the 2-h urine NGAL measurement, the area under the curve was 0.95, sensitivity was 0.82, and the specificity was 0.90 for prediction of AKI using a cutoff value of 100 ng/ml. The 2-h urine NGAL levels correlated with severity and duration of AKI, length of stay, dialysis requirement, and death.

Conclusions: Accurate measurements of urine NGAL are obtained using the ARCHITECT® platform. Urine NGAL is an early predictive biomarker of AKI severity after CPB.

	Introduction

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Cardiopulmonary bypass (CPB) surgery is the most frequent major surgical procedure performed in hospitals worldwide, with well over a million operations undertaken each year in adults alone (1). Acute kidney injury (AKI), previously referred to as acute renal failure, is a frequent and serious complication encountered in 30% to 50% of subjects after CPB (2,3). AKI requiring dialysis occurs in up to 5% of these cases, in whom the mortality rate approaches 80%, and is the strongest independent risk factor for death after CPB, with an odds ratio of 7.9 (4). Even minor degrees of postoperative AKI, as manifest by only a 0.2 to 0.3 mg/dl rise in serum creatinine from baseline, predict a significant increase in short-term mortality (5,6). AKI after cardiac surgery is also associated with a number of adverse outcomes, including prolonged intensive care and hospital stay, dialysis dependency, diminished quality of life, and increased long-term mortality (7–9).

Clinical investigations have identified several risk factors associated with the development of AKI after CPB, the majority related to either impaired renal perfusion or decreased renal reserve, and have resulted in the development of clinical scoring systems for the prediction of AKI (10–13). However, these tools have not been validated across medical centers, and have focused primarily on identifying the small number of high-risk, dialysis-requiring subjects. Concomitant advances in the basic sciences have illuminated the pathogenesis of AKI and have paved the way for successful therapeutic approaches in animal models (14). However, translational research efforts for the identification of effective therapeutic strategies in humans with AKI have yielded disappointing results (2,15). A major reason for the failure to find an effective treatment in patients is the paucity of early biomarkers for AKI, akin to troponins in acute myocardial disease (16). The availability of effective biomarkers may lead to improved efforts at ameliorating the course of AKI or preventing further renal injury. However, in current clinical practice, the gold standard for identification and classification of AKI is dependent on serial serum creatinine measurements (17), which are especially unreliable during acute changes in kidney function (15,16).

We used a genome-wide interrogation strategy to identify kidney genes that are induced very early after AKI in animal models, whose protein products might serve as novel early biomarkers. We identified neutrophil gelatinase-associated lipocalin (NGAL) as one of the most upregulated genes in the kidney soon after ischemic injury (18–20). NGAL protein was also markedly induced in kidney tubule cells and easily detected in the plasma and urine in animal models of ischemic and nephrotoxic AKI (18–22). The expression of NGAL protein was also dramatically increased in kidney tubules of humans with ischemic, septic, and post-transplant AKI (23,24). Importantly, NGAL in the urine was found to be an early predictive biomarker of AKI in a variety of acute clinical settings (25). In a cohort of 20 subjects who developed AKI 2 to 3 d after cardiac surgery, urine NGAL measured by a research enzyme-linked immunosorbent assay (ELISA) was elevated within 2 to 6 h after CPB (16,26). Preliminary results using the research-based assay also suggest that urine NGAL measurements can predict AKI following contrast administration (27), kidney transplantation (28), hemolytic-uremic syndrome (29), lupus nephritis (30), and in critically ill subjects (31). The availability of a standardized clinical platform for NGAL measurements could revolutionize renal diagnostics, especially in intensive care situations (32). Therefore, the first objective of the present study was to determine whether an NGAL immunoassay developed for a standardized clinical platform (ARCHITECT® analyzer, Abbott Diagnostics) correlates with the research-based assay. The second objective was to determine the utility of the standardized NGAL immunoassay as a predictive biomarker of AKI after CPB in a large prospective cohort.

	Materials and Methods

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Patients and Study Design
This investigation was approved by the institutional review board of the Cincinnati Children's Hospital Medical Center. All children undergoing elective CPB for surgical correction or palliation of congenital heart lesions between January 2004 and June 2006 were prospectively enrolled. We obtained written informed consent from the legal guardian of every participant before enrollment. Exclusion criteria included preexisting renal insufficiency, diabetes mellitus, peripheral vascular disease, and use of nephrotoxic drugs before or during the study period. Preexisting renal insufficiency was defined as a serum creatinine level that was greater than the 90th percentile for the child's age and gender. Patients with a history of potential nephrotoxin use (including aminoglycosides, angiotensin inhibitors, and nonsteroidal anti-inflammatory drugs) during the preoperative day or the first two postoperative days were excluded because of potential confounding effects on urinary NGAL measurements.

We used the Risk Adjustment for Congenital Heart Surgery 1 consensus-based scoring system to categorize the complexity of surgery (33) (Table 1). This method of risk stratification has emerged as a widely accepted tool for the evaluation of differences in outcomes of surgery for congenital heart disease.

The primary outcome variable was the development of AKI, defined as a 50% or greater increase in serum creatinine from baseline. Other outcomes included percent change in serum creatinine, days in AKI, dialysis requirement, length of hospital stay, and mortality. Other variables we obtained included age, gender, ethnic origin, CPB time, previous heart surgery, and urine output.

In a pilot cross-sectional study, we measured NGAL concentrations with 136 urine samples (NGAL range, 0.3 to 815 ng/ml) and 6 calibration standards (NGAL range, 0 to 1000 ng/ml) to determine the correlation between the two assay methods described below. In a subsequent prospective study, serial urine samples from 196 children undergoing CPB were assayed for NGAL using the standardized clinical platform (ARCHITECT® analyzer, Abbott Diagnostics) to assess its ability to predict AKI and other adverse outcomes.

NGAL Analysis by Standardized Clinical Platform (ARCHITECT®)
The ARCHITECT® NGAL assay is currently under development. High affinity antibodies were generated toward distinct epitopes on NGAL and assay standards were prepared using human recombinant NGAL. The assay is a two-step (sandwich) assay using Chemiluminescent Microparticle Immunoassay technology. The ARCHITECT® assay had a functional sensitivity <2 ng/ml (20% coefficient of variation [CV], 95% confidence) and total CVs <5.0%.

NGAL Analysis by ELISA
The urine NGAL ELISA was performed using a commercially available assay (NGAL ELISA Kit 036; AntibodyShop, Grusbakken, Denmark) that specifically detects human NGAL. The assay was performed as per the manufacturer's protocol. Briefly, 100 µl of NGAL standards or diluted samples was applied on to the precoated microwells in duplicates. Microwells were then incubated for 1 h at room temperature and then washed with washing buffer. In succession, biotinylated NGAL antibody and HRP-streptavidin were incubated in the wells for 1 h each with shaking at 200 x g. TMB substrate was added for 10 min in the dark before adding stop solution. Finally, NGAL concentration was measured at 450 nm wavelength in each well with reference reading at 620 nm in blank wells. The intra-assay CV were 2.1% (range, 1.3% to 4.0%) and 3.0% (range, 1.2% to 4.0%) in urine and plasma, respectively. Interassay variation was 9.1% (range, 6.8% to 18.1%) and 8.2% (range, 2.2% to 11.2%) in urine and plasma, respectively. Urine creatinine was measured using quantitative colorimetric Microplate Assay Kit (Oxford Biomedical Research, Oxford, MA) to standardize urinary NGAL for changes in urine concentration. Urinary NGAL excretion is presented as the amount of urinary NGAL in ng per ml urine as well as in ng per mg of urine creatinine to correct for differences in NGAL due to urine dilution. All measurements were made in triplicate. The laboratory investigators were blinded to the sample sources and clinical outcomes until the end of the study.

Statistical Analysis
Statistical analysis for Table 2 was performed using SAS, version 9.2. Either a two-sample t test or Mann-Whitney rank sum test was used for continuous variables and ² or Fisher's exact test was used for categorical variables. The associations between NGAL and change in creatinine (Delta creat), duration of AKI (days), and hospital length of stay were assessed by Spearman Rank Order correlation analysis. Correlations between NGAL and AKI outcome, dialysis requirement, and death were performed using a logistic correlation. Multivariate stepwise multiple logistic regression analysis was undertaken to assess predictors of adverse clinical outcomes (duration of AKI and hospital length of stay). Potential independent predictor variables included age, gender, CPB time, and urinary NGAL values at 2, 4, and 6 h after CPB. The area under the curve (AUC) was calculated from a standard receiver-operating characteristic plot. Spearman Rank Order correlations were performed using the website www.wessa.net/rankcorr.wasp (v1.1.21-r4), and the logistic correlations were performed using JMP (v5.0.1a). An AUC of 0.5 is no better than expected by chance, whereas a value of 1.0 signifies a perfect biomarker. A P 0.05 was considered statistically significant.

	Results

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View larger version (11K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 1. Correlation between urine NGAL measurements obtained by ARCHITECT® platform and research-based NGAL ELISA assay (AntibodyShop).

View larger version (13K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 2. Serum creatinine measurements obtained at various time points post-CPB. AKI, acute kidney injury, defined as a 50% increase in serum creatinine from baseline. Values are mean ± SEM and are shown in Table 2. *P < 0.05 comparing AKI versus no AKI groups.

View larger version (12K): [in this window] [in a new window] [as a PowerPoint slide]   Figure 3. Urine NGAL measurements obtained by ARCHITECT® assay at various time points post-CPB. AKI, acute kidney injury, defined as a 50% increase in serum creatinine from baseline. Values are mean ± SEM and are shown in Table 3. *P < 0.05 comparing AKI versus no AKI groups.

To test the hypothesis that urine NGAL levels measured soon after CPB could be used to predict eventual clinical outcomes, the Spearman Rank Order correlation analysis or logistic regression analysis was performed as appropriate. The results are illustrated in Table 6. The 2, 4, and 6 h urine NGAL levels strongly correlated with percent change in serum creatinine, duration of AKI, and length of hospital stay (all P < 0.0001). The 2 h urine NGAL levels also correlated with subsequent dialysis requirement (r = 0.48, P = 0.01) as well as mortality (r = 0.53, P = 0.01).

To assess the utility of urine NGAL measurements at varying cutoff values to predict AKI, conventional receiver-operating characteristic curves were generated, and the AUCs calculated. Table 7 lists the derived sensitivities and specificities at different cutoff concentrations, and the calculated AUCs at each time point are shown in Table 3. For urine NGAL at 2 h after CPB, sensitivity and specificity were optimal at the 100 ng/ml cutoff, with an AUC of 0.93 for the prediction of AKI, indicative of an excellent biomarker. Using a similar approach, the 2 h urine NGAL was also an excellent biomarker for the prediction of dialysis requirement (AUC = 0.86) and mortality (AUC = 0.91). However, the number of events was small (n = 4 for dialysis requirement and n = 3 for mortality).

	Discussion

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Serum creatinine is an inadequate marker for AKI (25). First, substantial losses of glomerular filtration rate (GFR) may occur before an increase in serum creatinine will be measured. Second, serum creatinine does not accurately depict kidney function until a steady state has been reached, which may require several days. Although animal studies have shown that AKI can be prevented and/or treated by several maneuvers, these must be instituted very early after the insult, well before the rise in serum creatinine. Our study indicates that monitoring of urine NGAL levels can provide a very early warning to providers of clinical care. The urine NGAL levels measured by the ARCHITECT® assay at several early time points after CPB were excellent biomarkers for the subsequent development of AKI and its complications. This assay is easy to perform with no manual pretreatment steps, a first result available within 35 min, and it requires only 150 µl of urine.

This study lends substantial support to our previous findings in a small cohort of 20 subjects who developed AKI 2 to 3 d after cardiac surgery, in whom both urine and plasma NGAL measured by a research ELISA was elevated within 2 to 6 h after CPB (16). Human NGAL, a member of the lipocalin superfamily, was initially described as a 25 kD protein covalently bound to gelatinase in neutrophils (34). NGAL expression is induced in injured epithelia, including lung, colon, and especially kidney (18–25). Emerging experimental and clinical evidence indicates that, in the early phases of AKI from diverse etiologies, NGAL accumulates within two distinct pools, namely, a renal and a systemic pool. Gene expression studies in AKI have clearly demonstrated rapid and massive upregulation of NGAL mRNA in the thick ascending limb of Henle's loop and the collecting ducts, with resultant synthesis of NGAL protein in the distal nephron (the renal pool) and secretion into the urine where it comprises the major fraction of urinary NGAL (35,36). In addition, AKI results in increased NGAL mRNA expression in distant organs, especially the liver and lung, and the overexpressed NGAL protein is most likely released into the circulation and constitutes the systemic pool (35–37).

Our study has several strengths. First, we prospectively recruited a relatively homogeneous cohort of pediatric subjects in whom the only obvious etiology for AKI would be the result of CPB. These patients comprise an ideal and important population for the study of AKI biomarkers because they do not exhibit common comorbid variables that complicate similar studies in adults, such as diabetes, hypertension, atherosclerosis, and nephrotoxin use (38). Second, all subjects started with normal kidney function, and the study design allowed for the precise temporal definition of altered urine NGAL concentrations and a direct comparison with subsequent changes in serum creatinine. Our results clearly indicate that urine NGAL is a powerful early biomarker of AKI that precedes the increase in serum creatinine by several hours to days. The magnitude of rise supports the notion that urine NGAL is a highly discriminatory biomarker with a wide dynamic range and cutoff values that allow for easy risk stratification. Third, this is the first example of how a standardized clinical laboratory platform (ARCHITECT®) may be useful for predicting AKI using urine samples. The majority of biomarkers of AKI described thus far have been measured in the urine (25). Urinary diagnostics have several advantages, including the noninvasive nature of sample collection and the reduced number of interfering proteins. Fourth, the results obtained using the ARCHITECT® platform were independent of changes in urinary concentration and were equally applicable after correction for urine creatinine measurements.

This study has important limitations. First, it is a single-center study of pediatric subjects with congenital heart defects undergoing elective CPB. Our results, although provocative and of clear statistical significance, will certainly need to be validated in a larger randomized prospective trial, including adults with the usual confounding variables and comorbid conditions that normally accumulate with increasing age. Second, ours was a cohort with normal kidney function at recruitment, and it will be important to confirm our findings in documented high-risk settings, such as preexisting kidney dysfunction, diabetes mellitus, and concomitant nephrotoxic drug use. Third, it is acknowledged that, although all recruited subjects had normal serum creatinine measurements before surgery, an estimation of GFR to document normal kidney function was not made. However, estimation of GFR in children using serum creatinine or creatinine-based equations is fraught with imprecision (39). Fourth, in addition to NGAL, simultaneous examination of other urinary biomarkers as potential predictors of AKI may be informative (25). It is possible that a collection of other strategically selected candidates along with NGAL will prove of value for early and rapid diagnosis of AKI.

What is the potential clinical utility of our findings? Ideally, an early elevation in urine NGAL would trigger an immediate paradigm shift in the clinical management of the patient. At the very least, clinicians informed of such a situation would be aware of the potential for development of clinical AKI, and biomarkers, such as NGAL, may add substantively to existing clinical scoring systems for AKI prediction. Such patients would deserve closer monitoring with respect to blood pressure, urine output, and renal perfusion. Every effort to monitor postoperative intravascular status and to optimize hydration and renal perfusion would be deployed. These subjects would benefit from the diligent avoidance of nephrotoxins. The ability to predict which patients will develop AKI after CPB could enable early initiation of interventions to change the dismal outcomes associated with this all-too-common clinical problem. For example, earlier intervention with renal replacement therapy may be strongly considered for subjects with elevated biomarker levels who are developing fluid overload but will not display increased serum creatinine for several days due to hemodilution and time required for reestablishment of a steady state. The availability of promising early biomarkers may enable the timely initiation of interventions, such as atrial natriuretic peptide (40) and insulin-like growth factor (41) that have been successful in smaller, phase II level efficacy studies but not in larger phase III trials. Possibly, these interventions would have been successful if they were initiated at the onset of AKI (as determined by predictive biomarkers) rather than waiting several days for serum creatinine to rise. In addition, animal studies have identified, and continue to reveal, novel therapies, such as growth factors, anti-apoptotic, anti-inflammatory, and anti-oxidant approaches that are effective in early AKI, before the rise in serum creatinine (14). The availability of a standardized commercial platform for urinary NGAL determination will enable these safe and highly promising agents to be investigated in humans with AKI.

	Disclosures

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None.

	Acknowledgments

 
This work was supported in part by a restricted research grant from Abbott Diagnostics. P.D. is supported by grants from the NIH/NIDDK (RO1-DK53289, P50-DK52612, R21-DK070163), a Grant-in-Aid from the American Heart Association Ohio Valley Affiliate, and a Translational Research Initiative Grant from Cincinnati Children's Hospital Medical Center.

Abbott Diagnostics has signed an exclusive licensing agreement with Cincinnati Children's Hospital and Columbia University for developing urine NGAL as a biomarker of acute renal failure.

The authors thank our patients and their families for their participation.

	Footnotes

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

Access to UpToDate on-line is available for additional clinical information at http://www.cjasn.org/

Received September 24, 2007. Accepted February 4, 2008.

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