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This article has been corrected. Correction in: Oncotarget. 2018; 9:9555.

Predictive value of post-procedural early (within 24 h) increase in cystatin C for contrast-induced acute kidney injury and mortality following coronary angiography or intervention

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Oncotarget. 2017; 8:109762-109771. https://doi.org/10.18632/oncotarget.19034

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Yong Liu, Kai-Hong Chen, Shi-Qun Chen, Li-Ling Chen, Chong-Yang Duan, Kun Wang, Xiao-Sheng Guo, Hua-Long Li, Wei-Jie Bei, Kai-Yan Lin, Ping-Yan Chen, Ying Xian, Ning Tan, Ying-Ling Zhou, Qing-Shan Geng and Ji-Yan Chen _

Abstract

Yong Liu1,*, Kai-Hong Chen2,*, Shi-Qun Chen1,3,*, Li-Ling Chen1,2,*, Chong-Yang Duan4,*, Kun Wang1,5,*, Xiao-Sheng Guo1, Hua-Long Li1, Wei-Jie Bei1, Kai-Yan Lin1,3, Ping-Yan Chen4, Ying Xian6, Ning Tan1, Ying-Ling Zhou1,3, Qing-Shan Geng1 and Ji-Yan Chen1

1 Department of Cardiology, Guangdong Cardiovascular Institute, Guangdong Key Laboratory of Coronary Disease Prevention, Guangdong General Hospital, Guangdong Academy of Medical Sciences, School of Medicine, South China University of Technology, Guangzhou, China

2 Department of Cardiology, Longyan First Affiliated Hospital of Fujian Medical University, Longyan, Fujian Province, China

3 Department of Cardiology, Guangdong General Hospital Zhuhai Hospital, Zhuhai, Guangdong, China

4 National Clinical Research Center for Kidney Disease, State Key Laboratory of Organ Failure Research, Department of Biostatistics, School of Public Health and Tropical Medicine, Southern Medical University, Guangzhou, China

5 Southern Medical University, Guangzhou, Guangdong, China

6 Duke Clinical Research Institute, Durham, NC, USA

* These authors contributed equally to this work.

Correspondence to:

Ji-Yan Chen, email:

Qing-Shan Geng, email:

Ying-Ling Zhou, email:

Keywords: cystatin C, coronary angiography, percutaneous coronary intervention, contrast-induced acute kidney injury

Received: March 03, 2017 Accepted: May 16, 2017 Published: July 06, 2017

Abstract

Objective: To investigate the predictive value of post-procedural early (within 24 h) increase in cystatin C for contrast-induced acute kidney injury (CI-AKI) and all-cause mortality following coronary angiography or intervention.

Methods: We prospectively investigated 1042 consecutive patients with both baseline and early post-procedural cystatin C measurement undergoing coronary angiography or intervention. CI-AKI was defined as an increase ≥0.3 mg/dL or >50% in serum creatinine from baseline within 48 h post-procedure. Mean follow-up was 2.26 years.

Results: Overall, the patients had a CI-AKI incidence was 3.6% (38/1042), mean serum creatinine of 87 µmol/L. Compared with Mehran risk score, post-procedural early absolute increase (AUC: 0.584 vs. 0.706, P = 0.060) and relative increase (AUC: 0.585 vs. 0.706, P = 0.058) in cystatin C had poorer predictive value for CI-AKI. According to multivariate analysis, post-procedural significant early increase (≥0.3 mg/dL or ≥10%) in cystatin C developed in 231 patients (22.2%), was not independent predictor of CI-AKI (adjusted OR: 1.23, 95% CI, 0.56–2.69, P = 0.612), and long-term mortality (adjusted HR: 0.90; P = 0.838).

Conclusions: Our data suggested post-procedural early increase (within 24 h) in cystatin C was not effective for predicting CI-AKI or all-cause mortality following coronary angiography or intervention among patients at relative low risk of CI-AKI, the negative finding of poor predictive value should be further evaluated in larger multicenter trials.


Introduction

Contrast-induced acute kidney injury (CI-AKI) is a common complication after percutaneous coronary intervention (PCI) and is associated with prolonged hospital stay, increased medical costs, and increased risk of adverse clinical outcomes [1, 2]. Since effective treatment measures for CI-AKI have not been established and the treatment window is narrow, early identification of patients at high risk of CI-AKI is important [3].

Serum creatinine (SCr) is a common index used to evaluate renal function and define CI-AKI. However, SCr concentration is affected by muscle mass, age, sex, and diet, and may not change until a significant loss of renal function [4-6]. Therefore, SCr concentration could be unreliable and overestimate the estimated glomerular filtration rate (eGFR).

Cystatin C, another biomarker to evaluate renal function, is produced at a constant rate by nucleated cells and reabsorbed in the proximal renal tubules [7]. Compared with SCr, the concentration of cystatin C is less affected by muscle mass, age, sex, and diet, and its half-life is 3 times shorter [8, 9], allowing for the reliable and early detection of changes in cystatin C levels in blood. Some previous studies indicated that the relative increase of cystatin C is a sensitive early biomarker of CI-AKI after contrast exposure [10, 11]. By contrast, other studies reported a low predictive value of CI-AKI [12, 13]. Previous studies have focused on specific patient groups (e.g. chronic kidney disease), but the association of cystatin C with CI-AKI in more general patient populations remains unknown. Therefore, the purpose of our study was to analyze the association of post-procedural early (within 24 h) increase in cystatin C with CI-AKI and long-term all-cause mortality following coronary angiography or intervention.

Results

Clinical characteristics

A total of 1042 patients were included in the final analysis (mean age 62.87 ± 10.35 years, mean creatinine clearance rate 75.12 ± 26.24 mL/min, and mean cystatin C 1.20 ± 0.47 mg/L), and 297(28.5%) patients presented with pre-existing chronic kidney disease (CKD), creatinine clearance <60 ml>Figure 1.

Patients’ baseline characteristics are listed in Table 1 and Table 2. Overall, 38 patients (3.6%) developed CI-AKI. Compared to patients without CI-AKI, patients with CI-AKI were older. Furthermore, those in the CI-AKI group had a lower creatinine clearance rate and higher Mehran risk score (Table 1).

In addition, 231 patients (22.2%) demonstrated a significant Δcystatin C. These patients were also more likely to be older and to have renal insufficiency, anemia, and higher Mehran risk score. However, the medication therapy, procedure process, and other demographic characteristics and biochemical parameters were similar between the two groups (Table 2). The incidence of CI-AKI did not differ between patients with and without a significant Δcystatin C (3.9% vs. 3.6%, respectively; P=0.819). Similar results were found in other in-hospital outcomes (Table 3).

Table 1: Characteristics of patients with or without CI-AKI

Characteristic

All patients

CI-AKI

Non-CI-AKI

P value

n= 1042

n = 38

n= 1004

Age

62.87±10.35

68.08±10.05

62.67±10.31

0.002

Sex (male)

784 (75.2%)

23 (60.5%)

761 (75.8%)

0.032

Serum creatinine, µmol/L

Baseline

87.22±38.23

97.92±45.57

86.82±37.89

0.079

Within 24 h post-procedure

88.82±34.57

138.28±56.17

86.94±32.05

<0.001

Within 48 h post-procedure

93.76 ± 46.57

130.72±67.82

90.70±43.09

0.005

Within 72 h post-procedure

105.23 ± 95.94

149.73±146.97

100.12±88.66

0.413

Serum cystatin C, mg/L

Baseline

1.20 ± 0.47

1.56±0.60

1.18±0.46

<0.001

Within 24 h post-procedure

1.16±0.49

1.65±0.62

1.14±0.48

<0.001

Within 48 h post-procedure

1.20 ± 0.51

1.51±0.63

1.18±0.49

0.002

Creatinine clearance rate, ml/min

75.12±26.24

67.27±38.28

75.42±25.65

0.201

>90

242 (23.3%)

6 (15.8%)

236 (23.6%)

<0.001

60-90

501 (48.2%)

10 (26.3%)

491 (49.0%)

30-60

274 (26.3%)

20 (52.6%)

254 (25.3%)

<30

23 (2.2%)

2 (5.3%)

21 (2.1%)

Mehran risk score

4.54±3.60

8.20±5.50

4.41±3.45

<0.001

£5

778 (77.0%)

15 (42.9%)

763 (78.2%)

<0.001

6-10

176 (17.4%)

10 (28.6%)

166 (17.0%)

11-15

41 (4.1%)

4 (11.4%)

37 (3.8%)

≥16

16 (1.6%)

6 (17.1%)

10 (1.0%)

Δcystatin C ≥0.3 mg/L within 24 h

76 (7.3%)

6 (15.8%)

70 (7.0%)

0.040

Δcystatin C ≥10% within 24 h

231 (22.2%)

9 (23.7%)

222 (22.1%)

0.819

Δcystatin C ≥0.3 mg/L or ≥10% within 24 h

231 (22.2%)

9 (23.7%)

222 (96.1%)

0.819

Δcystatin C ≥0.5 mg/L within 24 h

28 (2.7%)

5 (13.2%)

23 (2.3%)

<0.001

Δcystatin C ≥25% within 24 h

97 (9.3%)

7 (18.4%)

90 (9.0%)

0.049

Δcystatin C ≥0.5 mg/L or ≥25% within 24 h

97 (9.3%)

7 (18.4%)

90 (9.0%)

0.049

Abbreviations: CI-AKI=contrast-induced acute kidney injury.

Table 2: Characteristics of patients with or without significant Δcystatin C

Variables

All patients

Significant Δcystatin C

Non-significant Δcystatin C

P value

n= 1042 n= 231 n= 811

Demographic variables

Age, years

62.87±10.35

61.26±10.51

63.33±10.26

0.007

Age >75 years

116 (11.1)

17 (7.4)

99 (12.2)

0.039

Men

784 (75.2)

171 (74.0)

613 (75.6)

0.628

Weight, kg

65.70±11.02

65.61±10.98

65.98±11.20

0.654

Smokers

389 (37.3)

94 (40.7)

295 (36.4)

0.255

Hypertension

608 (58.3)

127 (55.0)

481 (59.3)

0.239

Diabetes mellitus

260 (25.0)

62 (26.8)

198 (24.5)

0.464

Anemia

365 (35.6)

67 (29.6)

298 (37.3)

0.034

Dyslipidemia

157 (15.1)

32 (13.9)

125 (15.4)

0.559

Congestive heart failure

119 (11.5)

18 (8.0)

101 (12.5)

0.057

Previous MI

125 (12.0)

30 (13.0)

95 (11.7)

0.599

Previous CABG

11 (1.1)

3 (1.3)

8 (1.0)

0.682

Biochemical parameters

SBP, mmHg

129.81 ±18.90

130.39±20.49

129.64±18.43

0.616

Hypotension

14 (1.3)

5 (2.2)

9 (1.1)

0.221

LVEF

59.89±12.67

59.94±12.78

59.69±12.33

0.804

LVEF <40%

82 (9.7)

19 (9.9)

63 (9.6)

0.902

Baseline SCr, μmol/L

87.22±38.23

84.81±29.22

87.91±40.42

0.195

Baseline CrCl, mL/min

75.12±26.24

78.34±26.14

74.20±26.21

0.034

HbA1c, %

6.51±1.27

6.51±1.17

6.51±1.30

0.949

Hemoglobin, g/dL

133.87±15.40

134.53±16.61

133.69±15.04

0.466

Total cholesterol, mmol/L

4.38 ± 1.11

4.45±1.21

4.37 ± 1.08

0.359

HDL-C, mmol/L

0.93±0.31

0.93 ± 0.33

0.93±0.30

0.992

LDL-C, mmol/L

2.56±0.92

2.62 ± 1.08

2.54 ± 0.87

0.311

Mehran risk score

4.54±3.60

4.07 ± 3.43

4.67 ± 3.64

0.027

Medication Therapy

Diuretic

132 (12.7)

29 (12.6)

103 (12.7)

0.953

ACEI/ARB

923 (88.6)

203 (87.9)

720 (88.8)

0.704

β-Blockers

942 (90.4)

205 (88.7)

736 (90.9)

0.332

Calcium channel blockers

186 (17.9)

47 (20.3)

139 (17.2)

0.268

Procedure performed

Coronary lesion

1.88±1.18

1.81±1.19

1.90±1.17

0.287

Emergency PCI

16 (1.5%)

4 (1.7%)

12 (1.5%)

0.784

IABP

7 (0.7%)

1 (0.4%)

6 (0.7%)

0.614

No. of stent used

1.41 ± 1.25

1.37±1.20

1.42±1.27

0.675

Total stent length, mm

34.92±33.59

34.62±32.30

35.01±33.97

0.884

Procedure duration, min

64.54±45.83

63.56±46.75

64.82±45.59

0.718

Contrast volume, mL

117.98±64.80

117.90±66.40

118.01±64.38

0.982

Hydration volume, mL

697.16±370.88

680.80±355.58

701.85±375.23

0.447

Abbreviations: ACEI/ARB = angiotensin converting enzyme inhibitor/angiotensin receptor blocker; CABG = coronary artery bypass grafting; CrCl = creatinine clearance ; eGFR = estimated glomerular clearance rate; HbA1c = hemoglobin A1c; HDL-C = high-density lipoprotein cholesterol; IABP = intra-aortic balloon pump; LDL-C = low-density lipoprotein cholesterol; LVEF = left ventricular ejection fraction; MI = myocardial infarction; PCI = percutaneous coronary intervention; SBP = systolic blood pressure; SCr = serum creatinine.

Table 3: In-hospital outcomes of the two groups

All patients

Significant Δcystatin C (≥0.3 mg/dL or ≥10%)

Non-significant Δcystatin C

P value

CI-AKI

38 (3.6)

9 (3.9)

29 (3.6)

0.819

Mortality

2 (0.2)

0 (0.0)

2 (0.2)

0.450

AHF

7 (0.7)

0 (0.0)

7 (0.9)

0.155

RRT

4 (0.4)

0 (0.0)

4 (0.5)

0.284

Re-AMI

1 (0.1)

0 (0.0)

1 (0.1)

0.593

Arrhythmia

7 (0.7)

1 (0.4)

6 (0.7)

0.614

Stroke

16 (1.5)

5 (2.2)

11 (1.4)

0.379

Bleeding

4 (0.4)

2 (0.9)

2 (0.2)

0.180

Abbreviations: AHF= acute heart failure; CI-AKI = contrast-induced acute kidney injury; RRT = renal replacement therapy; Re-AMI = recurrent acute myocardial infarction; IABP = intra-aortic balloon pump.

Flow

Figure 1: Flow diagram of the selection process

Association between cystatin C and CI-AKI

ROC curve analysis revealed that early absolute or relative increase in cystatin C (as Δcystatin C, within 24 h) had poorer predictive value than Mehran risk score for CI-AKI (AUC=0.584 vs. 0.706, P=0.060; AUC=0.585 vs. 0.706, P=0.058; respectively) (Figure 2). We added Cystatin C in Mehran risk model, and the result shows that Cystatin C can’t significantly improve the prediction value (Supplementary Figure 1).

Receiver

Figure 2: Receiver operating characteristic curves for contrast-induced acute kidney injury

After controlling for other confounders, including age >75 years, creatinine clearance <60 ml>60kg, smoke, C-reactive protein (CRP)>3mmol/l and hydration volume ≤960 mL, multivariate logistic regression results revealed that significant Δcystatin C (≥0.3 mg/dL or ≥10%) was not associated with CI-AKI (OR=0.88, 95%CI, 0.32-2.41, P=0.798), so did Δcystatin C absolute increase ≥0.5 mg/L or relative increase≥25% (OR=2.15, 95%CI, 0.68~6.81, P=0.195) (Table 4).

Table 4: Multivariate analyses for predictors of contrast-induced nephropathy (CIN)

Variables

Adjusted OR

95% CI

P value

ΔCystatin C >0.3 mg/L to predict CIN

1.82

0.50–6.62

0.362

ΔCystatin C >10% to predict CIN

0.88

0.32–2.41

0.798

ΔCystatin C >0.3 mg/L or 10% to predict CIN

0.88

0.32–2.41

0.798

ΔCystatin C >0.5 mg/L to predict CIN

5.28

1.36~20.57

0.016

ΔCystatin C >25% to predict CIN

2.15

0.68~6.81

0.195

ΔCystatin C >0.5 mg/L or 25% to predict CIN

2.15

0.68~6.81

0.195

CIN was adjusted for age >75 years, creatinine clearance <60 ml>60kg, smoking, C-reactive protein >3mmol/L, and hydration volume ≤960 mL.

Association of cystatin C with long-term outcomes

The mean follow-up period was 2.26 years. Kaplan-Meier curve analysis revealed that significant Δcystatin C was not associated with increased long-term mortality (P=0.627) (Figure 3). After adjusting for confounders, including age, diabetes, creatinine clearance, female gender, weight>60kg, smoke, C-reactive protein (CRP) >3mmol/l and LVEF, significant Δcystatin C (≥0.3 mg/dL or ≥10%) was not an independent risk factor for long-term mortality (HR=1.08, 95%CI, 0.34-3.43, P=0.902) (Figure 4).

Kaplan-Meier

Figure 3: Kaplan-Meier curve for long-term mortality

Multivariate

Figure 4: Multivariate Cox regression analysis for long-term mortality

Discussion

To our knowledge, this study is the largest to date to investigate the relation of change in cystatin C to CI-AKI and long-term mortality in patients undergoing coronary angiography or intervention. Because CI-AKI is associated with renal and cardiovascular adverse events and long-term mortality, its early identification is critical. However, our data indicated that early significant increase in cystatin C did not have good predictive value for CI-AKI and long-term mortality.

CI-AKI is a common and serious complication after contrast exposure, which can affect up to 50% of patients with additional risk factors, such as administration of a high dose of CM, undergoing emergency PCI, and chronic kidney disease [3]. However, the incidence of CI-AKI in our analysis (3.6%) was lower than that in previous reports. Our study population was not limited to patients with acute coronary syndrome. Furthermore, some patients who underwent coronary angiography without stent implantation may have received a low dose of CM (30-50 ml) during the procedure. In addition, fewer than half of patients had chronic kidney disease. All of the abovementioned reasons may have contributed to the lower CI-AKI incidence observed in this study.

Cystatin C, a 13-kDa cysteine protease inhibitor, is produced at a constant rate by nucleated cells. Compared with SCr, cystatin C is reabsorbed and almost completely catabolized in the proximal renal tubules. Due to its low molecular weight and positive charge at physiological pH, the serum concentration of cystatin C is determined by glomerular filtration and less influenced by age, sex, muscle mass, and nutrition than SCr. In addition, cystatin C is only present in the extracellular space, leading to its quicker increase and shorter half-life in serum [8, 9]. Therefore, the concentration of cystatin C can rapidly increase after CM exposure, and it had been postulated to be valuable for the early prediction of CI-AKI.

Previous studies demonstrated that Δcystatin C was an independent predictor of CI-AKI. A study including a total of 204 patients undergoing primary angioplastyfound that cystatin C relative increase ≥10% within 72 h had a good predictive value for CI-AKI, with 96.30% sensitivity and 67.23% specificity [11]. Similarly, a recent prospective analysis further confirmed the value of Δcystatin C for CI-AKI in patients undergoing elective coronary angiography [14]. Furthermore, Kim et al demonstrated similar results in patients with peripheral artery disease after contrast exposure [10]. Although cystatin C rapidly peaks within 24 h after contrast exposure and decreases thereafter, all of these previous studies analyzed Δcystatin C within 48-72h, which might influence its predictive value. By contrast, an observational study by Ribichini et al including 166 patients who underwent coronary angioplasty analyzed the change in cystatin C within 24 h and indicated that Δcystatin C >10% within 24 h was not associated with an elevated risk of CI-AKI [12]. Furthermore, the early changes in cystatin C levels (12 h from baseline) were not superior to changes in SCr levels for predicting CI-AKI in patients who underwent coronary angioplasty. The variable definition of CI-AKI, differences in treatment or measurement time, and disparate patient populations may all have contributed to these conflicting results. To overcome these obstacles, the present study included a relatively large population of patients who underwent cardiac catheterization and analyzed the predictive value of Δcystatin C within 24 h for CI-AKI.

The increase in serum cystatin C levels after ST-elevation myocardial infarction could also be a predictor of medium-term major adverse cardiovascular events [15]. A meta-analysis of human studies demonstrated that patients with elevated cystatin C levels prior to the diagnosis of acute kidney injury have worse outcomes. However, the analysis failed to identify a consensus cut-off value to define cystatin C level elevation [16], potentially because cystatin C is not only a sensitive marker of kidney function but also associated with atherosclerosis and cardiac structural abnormalities. Furthermore, cystatin C has unforeseen toxic effects that also contribute to the strength of its association with mortality and cardiovascular risk [17]. By contrast, we found that an early increase in cystatin C (relative or absolute 24-h post-procedural change) did not predict CI-AKI or long-term adverse outcomes. Additional comprehensive studies with larger samples are needed to determine whether early changes in cystatin C levels are a better predictor for CI-AKI and major adverse cardiovascular events.

We acknowledge several limitations of our study. First, this prospective observational study was conducted at a single center with a limited sample size, which prevents these findings from being extended to other patient populations until they are confirmed by larger multicenter clinical trials. Second, variation of post-procedural cystatin C measurement times may have led to peak levels of cystatin C being missed. Third, the high missing data rate (70%) of systemic cystatin C measurement (baseline or post-procedural) increased the bias of the population selection, which further limits the extension of our findings. Fourth, approximately half of patients were discharged at 48 h after coronary angiography or interventions, which may have led to an underestimation of the true incidence of CI-AKI. Fifth, the incidence of CI-AKI, which served as the primary end-point, was low among patients with low Mehran score and serum creatinine, and we did not have adequate data to investigate the contrast limit in high-risk patients. Sixthly, all the data of cystatin C did not come from urine sample, which may be more sensitive and early to detect CI-AKI, but come from blood sample. Finally, although we previously promoted the use of a hydration protocol, no strictly uniform protocol was applied in this observational study, which may have influenced the dynamic change of post-procedural cystatin C and the incidence of CI-AKI.

In conclusion, our data suggest that post-procedural early increase (within 24 h) in cystatin C is not effective for predicting CI-AKI or all-cause mortality following coronary angiography or intervention among patients at low risk of CI-AKI. The reverse finding of poor predictive value for post-procedural early increase in cystatin C needs further evaluation in larger multicenter trials.

Materials and Methods

Study population

This study included 3957 consecutive patients more than 18 years old who underwent coronary angiography or intervention according to the institutional protocol between January 2010 and October 2012 at Guangdong General Hospital. In accordance with the updated European guidelines on contrast media [3], the exclusion criteria included pregnancy, lactation, intravascular administration of a contrast medium (CM) within the previous 7 days or 3 days postoperation, no use of low-osmolality contrast agents, cardiovascular surgery or endovascular repair, end-stage renal disease or renal replacement, missing preoperative or postoperative creatinine, missing preoperative or postoperative cystatin C, malignancy, and no use of isotonic saline for hydration. Consequently, 1042 patients with both preoperative baseline and early postoperative (<24 h) measurement of cystatin c were included in the final study (Figure 1).

This study was performed according to the Declaration of Helsinki, and the ethics committee of the Guangdong General Hospital approved the study protocol. Written informed consent was obtained from the patients involved in the study.

Biochemical investigations

SCr concentration was measured at admission and within 24 h, 48 h, and 72 h after CM administration. Cystatin C was measured prior to the procedure and within 24 h after the procedure. Other biochemical indicators, such as hemoglobin (Hb) A1c, lipid profile, and Hb level, were measured in the morning prior to the procedure. The Cockcroft-Gault formula was used to calculate the eGFR [18].

Cardiac catheterization

The cardiac catheterization procedure was performed via a femoral or radial approach by experienced interventional cardiologists according to standard clinical practice. Non-ionic, low-osmolality CM was used for all patients (either Iopamiron® or Ultravist®, both 370 mg I/mL). Patients received a continuous intravenous infusion of isotonic saline at a rate of 1 mL/kg/h (0.5 mL/kg/h in cases of left ventricular ejection fraction <40% or severe congestive heart failure) for at least 2-12 h before and 6-24 h after the procedure. The use of drugs was based on the patient’s condition and PCI guidelines [19].

Clinical end-points and follow-up

The primary end-point of this study was the development of CI-AKI, defined as an absolute increase ≥0.3 mg/dL or a relative increase >50% from baseline SCr level within 48 h after contrast exposure [20]. Additional end-points included significant early absolute or relative increase in cystatin C (Δcystatin C), defined as an absolute increase ≥0.3 mg/dL or relative increase ≥10% from baseline within 24 h after contrast exposure, and all-cause mortality [10].

During the mean follow-up period of 2.26 years (interquartile range, 1.84-2.68 years), events were carefully monitored and recorded by trained nurses through office or telephone visits at 1, 6, 12, 24, 36, and 48 months after discharge.

Statistical analysis

For continuous variables, t-tests were used for normally distributed data (described as mean ± standard deviation), and the Wilcoxon rank-sum test was used for data with non-normal distribution (described as interquartile range). For categorical variables, χ2 test or Fisher’s exact test was used (described as absolute values and percentages). Receiver operating characteristic (ROC) curve analysis was conducted to assess the predictive value of Δcystatin C for CI-AKI. Area under the curve (AUC) values were compared between Δcystatin C and Mehran score by using MedCalc statistical software (MedCalc software, version 11.4, Mariakerke, Belgium) [21]. Multivariate logistic regression and Cox proportional hazards regression analyses were performed to identify the independent risk factors for CI-AKI and long-term mortality, respectively. The Kaplan-Meier method was used to describe the all-cause mortality by log-rank tests. All data analyses were performed using SAS version 9.4 (SAS Institute, Cary, NC, USA). A two-tailed P<0.05 was considered statistically significant.

Author contributions

Yong Liu, Kai-hong Chen, Shi-qun Chen, Ying-ling Zhou, Qing-shan Geng, and Ji-yan Chen conceived and designed the analysis; Yong Liu, Shi-qun Chen, and Li-ling Chen wrote the paper; Ying Xian modified the grammatical and stylistic rules. Chong-yang Duan, Shi-qun Chen, and Ping-yan Chen analyzed the data; Wei-jie Bei, Xiao-sheng Guo, and Kai-yan Lin collected the clinical data. Ning Tan and Ying Xian reviewed and revised the manuscript. All authors read and approved the final manuscript.

Conflicts of Interests

The authors declare that there is no conflict of interest.

Funding

This study was supported by Guangdong Provincial Cardiovascular Clinical Medicine Research Fund (Grant no. 2009X41 by Yong Liu and Ning Tan), Science and Technology Planning Project of Guangdong Province (PRECOMIN study by Yong Liu in 2011, grant No. 2008A030201002 by Ji-yan Chen, 2013b031800025 and 2016b020215130), and Guangdong Cardiovascular Institute.

References

1. Aubry P, Brillet G, Catella L, Schmidt A, Bénard S. Outcomes, risk factors and health burden of contrast-induced acute kidney injury: an observational study of one million hospitalizations with image-guided cardiovascular procedures. BMC Nephrol. 2016; 17:167. https://doi.org/10.1186/s12882-016-0385-5

2. Tsai TT, Patel UD, Chang TI, Kennedy KF, Masoudi FA, Matheny ME, Kosiborod M, Amin AP, Messenger JC, Rumsfeld JS, Spertus JA. Contemporary incidence, predictors, and outcomes of acute kidney injury in patients undergoing percutaneous coronary interventions: insights from the NCDR Cath-PCI registry. JACC Cardiovasc Interv. 2014; 7:1–9. https://doi.org/10.1016/j.jcin.2013.06.016

3. Stacul F, van der Molen AJ, Reimer P, Webb JA, Thomsen HS, Morcos SK, Almén T, Aspelin P, Bellin MF, Clement O, Heinz-Peer G, and Contrast Media Safety Committee of European Society of Urogenital Radiology (ESUR). Contrast induced nephropathy: updated ESUR Contrast Media Safety Committee guidelines. Eur Radiol. 2011; 21:2527–41. https://doi.org/10.1007/s00330-011-2225-0

4. American Society of Nephrology. American Society of Nephrology Renal Research Report. J Am Soc Nephrol. 2005; 16:1886–903. https://doi.org/10.1681/ASN.2005030285

5. Bellomo R, Ronco C, Kellum JA, Mehta RL, Palevsky P, and Acute Dialysis Quality Initiative workgroup. Acute renal failure - definition, outcome measures, animal models, fluid therapy and information technology needs: the Second International Consensus Conference of the Acute Dialysis Quality Initiative (ADQI) Group. Crit Care. 2004; 8:R204–12. https://doi.org/10.1186/cc2872

6. Wasung ME, Chawla LS, Madero M. Biomarkers of renal function, which and when? Clin Chim Acta. 2015; 438:350–57. https://doi.org/10.1016/j.cca.2014.08.039

7. Patel SS, Molnar MZ, Tayek JA, Ix JH, Noori N, Benner D, Heymsfield S, Kopple JD, Kovesdy CP, Kalantar-Zadeh K. Serum creatinine as a marker of muscle mass in chronic kidney disease: results of a cross-sectional study and review of literature. J Cachexia Sarcopenia Muscle. 2013; 4:19–29. https://doi.org/10.1007/s13539-012-0079-1

8. Onopiuk A, Tokarzewicz A, Gorodkiewicz E. Cystatin C: a kidney function biomarker. Adv Clin Chem. 2015; 68:57–69. https://doi.org/10.1016/bs.acc.2014.11.007

9. Briguori C, Visconti G, Rivera NV, Focaccio A, Golia B, Giannone R, Castaldo D, De Micco F, Ricciardelli B, Colombo A. Cystatin C and contrast-induced acute kidney injury. Circulation. 2010; 121:2117–22. https://doi.org/10.1161/CIRCULATIONAHA.109.919639

10. Kim GS, Ko YG, Shin DH, Kim JS, Kim BK, Choi D, Hong MK, Jang Y. Elevated serum cystatin C level is an independent predictor of contrast-induced nephropathy and adverse outcomes in patients with peripheral artery disease undergoing endovascular therapy. J Vasc Surg. 2015; 61:1223–30. https://doi.org/10.1016/j.jvs.2014.11.079

11. Yin L, Li G, Liu T, Yuan R, Zheng X, Xu G, Xu Y, Che J, Liu X, Ma X, Li F, Liu E, Chen X, et al. Probucol for the prevention of cystatin C-based contrast-induced acute kidney injury following primary or urgent angioplasty: a randomized, controlled trial. Int J Cardiol. 2013; 167:426–29. https://doi.org/10.1016/j.ijcard.2012.01.017

12. Ribichini F, Gambaro G, Graziani MS, Pighi M, Pesarini G, Pasoli P, Anselmi M, Ferrero V, Yabarek T, Sorio A, Rizzotti P, Lupo A, Vassanelli C. Comparison of serum creatinine and cystatin C for early diagnosis of contrast-induced nephropathy after coronary angiography and interventions. Clin Chem. 2012; 58:458–64. https://doi.org/10.1373/clinchem.2011.170464

13. Xu Q, Wang N, Duan S, Liu N, Lei R, Cheng W, Zhou SK. Serum cystatin c is not superior to serum creatinine for early diagnosis of contrast-induced nephropathy in patients who underwent angiography. J Clin Lab Anal. 2017; 31. https://doi.org/10.1002/jcla.22096

14. Kim BJ, Sung KC, Kim BS, Kang JH, Lee KB, Kim H, Lee MH. Effect of N-acetylcysteine on cystatin C-based renal function after elective coronary angiography (ENABLE Study): a prospective, randomized trial. Int J Cardiol. 2010; 138:239–45. https://doi.org/10.1016/j.ijcard.2008.08.013

15. Droppa M, Desch S, Blase P, Eitel I, Fuernau G, Schuler G, Adams V, Thiele H. Impact of N-acetylcysteine on contrast-induced nephropathy defined by cystatin C in patients with ST-elevation myocardial infarction undergoing primary angioplasty. Clin Res Cardiol. 2011; 100:1037–43. https://doi.org/10.1007/s00392-011-0338-8

16. Feng Y, Zhang Y, Li G, Wang L. Relationship of cystatin-C change and the prevalence of death or dialysis need after acute kidney injury: a meta-analysis. Nephrology (Carlton). 2014; 19:679–84. https://doi.org/10.1111/nep.12312

17. Shlipak MG, Sarnak MJ, Katz R, Fried LF, Seliger SL, Newman AB, Siscovick DS, Stehman-Breen C. Cystatin C and the risk of death and cardiovascular events among elderly persons. N Engl J Med. 2005; 352:2049–60. https://doi.org/10.1056/NEJMoa043161

18. Xun L, Cheng W, Hua T, Chenggang S, Zhujiang C, Zengchun Y, Tanqi L. Assessing glomerular filtration rate (GFR) in elderly Chinese patients with chronic kidney disease (CKD): a comparison of various predictive equations. Arch Gerontol Geriatr. 2010; 51:13–20. https://doi.org/10.1016/j.archger.2009.06.005

19. Wright RS, Anderson JL, Adams CD, Bridges CR, Casey DE Jr, Ettinger SM, Fesmire FM, Ganiats TG, Jneid H, Lincoff AM, Peterson ED, Philippides GJ, Theroux P, et al. 2011 ACCF/AHA focused update of the Guidelines for the Management of Patients with Unstable Angina/Non-ST-Elevation Myocardial Infarction (updating the 2007 guideline): a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines developed in collaboration with the American College of Emergency Physicians, Society for Cardiovascular Angiography and Interventions, and Society of Thoracic Surgeons. J Am Coll Cardiol. 2011; 57:1920–59. https://doi.org/10.1016/j.jacc.2011.02.009

20. Zeng X, McMahon GM, Brunelli SM, Bates DW, Waikar SS. Incidence, outcomes, and comparisons across definitions of AKI in hospitalized individuals. Clin J Am Soc Nephrol. 2014; 9:12–20. https://doi.org/10.2215/CJN.02730313

21. Mehran R, Aymong ED, Nikolsky E, Lasic Z, Iakovou I, Fahy M, Mintz GS, Lansky AJ, Moses JW, Stone GW, Leon MB, Dangas G. A simple risk score for prediction of contrast-induced nephropathy after percutaneous coronary intervention: development and initial validation. J Am Coll Cardiol. 2004; 44:1393–99. https://doi.org/10.1016/j.ja


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