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Abstract

French

Background:

Acute kidney injury (AKI) commonly occurs in patients with sepsis and acute respiratory distress syndrome (ARDS).

Objective:

To investigate whether statin treatment is protective against AKI in sepsis-associated ARDS.

Design:

Secondary analysis of data from Statins for Acutely Injured Lungs in Sepsis (SAILS), a randomized controlled trial that tested the impact of rosuvastatin therapy on mortality in patients with sepsis-associated ARDS.

Setting:

44 hospitals in the National Heart, Lung, and Blood Institute ARDS Clinical Trials Network.

Patients:

644 of 745 participants in SAILS who had available baseline serum creatinine data and who were not on chronic dialysis.

Measurements:

Our primary outcome was AKI defined using the Kidney Disease Improving Global Outcomes creatinine criteria. Randomization to rosuvastatin vs placebo was the primary predictor. Additional covariates include demographics, ARDS etiology, and severity of illness.

Methods:

We used multivariable logistic regression to analyze AKI outcomes in 511 individuals without AKI at randomization, and 93 with stage 1 AKI at randomization.

Results:

Among individuals without AKI at randomization, rosuvastatin treatment did not change the risk of AKI (adjusted odds ratio: 0.99, 95% confidence interval [CI]: 0.67-1.44). Among those with preexisting stage 1 AKI, rosuvastatin treatment was associated with an increased risk of worsening AKI (adjusted odds ratio: 3.06, 95% CI: 1.14-8.22). When serum creatinine was adjusted for cumulative fluid balance among those with preexisting stage 1 AKI, rosuvastatin was no longer associated worsening AKI (adjusted odds ratio: 1.85, 95% CI: 0.70-4.84).

Limitations:

Sample size, lack of urine output data, and prehospitalization baseline creatinine.

Conclusion:

Treatment with rosuvastatin in patients with sepsis-associated ARDS did not protect against de novo AKI or worsening of preexisting AKI.

Keywords

AKI acute renal failure statin sepsis ARDS

What was known before

Statins have been shown to prevent septic and ischemic acute kidney injury (AKI) in some animal models, and recent human data—including randomized trials—suggest potential benefit in prevention of contrast-induced AKI. However, it is not known whether statin therapy may be protective against sepsis-associated AKI in critically ill patients with acute respiratory distress syndrome (ARDS).

What this adds

Using data from Statins for Acutely Injured Lungs in Sepsis (SAILS), we found that administration of rosuvastatin did not prevent new-onset AKI and did not prevent worsening of existing AKI, after taking into account demographics, ARDS etiology, and severity of illness.

Introduction

Acute kidney injury (AKI) is a common and serious complication in patients with sepsis. Among critically ill patients, sepsis is estimated to be the primary trigger for ~40% to 50% of AKI cases.¹ Sepsis-associated AKI is associated with mortality of up to 50% to 60%, with a graded association between AKI severity and death.² There are limited therapeutic options in treating sepsis-associated AKI besides supportive care, including renal replacement therapies when indicated.

Statins have been shown to prevent septic and ischemic AKI in mouse models^3-5 and have been proposed as a novel treatment for AKI. Recent human studies have primarily focused on the effect of statin therapy on preventing AKI in patients undergoing coronary angiography⁶ and cardiac surgery.⁷ In this study, we sought to investigate the effect of statin therapy on sepsis-associated AKI in critically ill patients with the acute respiratory distress syndrome (ARDS).

Methods

Study Design and Population

We analyzed data from the Statins for Acutely Injured Lungs in Sepsis (SAILS) study from the National Heart, Lung, and Blood Institute ARDS Clinical Trials Network.⁸ SAILS was a multicenter, prospective, randomized controlled, double-blinded trial evaluating the effect of rosuvastatin therapy in critically ill patients with sepsis-associated ARDS. In total, 745 participants were enrolled from 44 hospitals from 2010 to 2013. The original SAILS design, protocol, and primary results have been described and published.⁸ Patients were eligible if they were receiving mechanical ventilation meeting the American/European Consensus Conference definition for Acute Lung Injury⁹ and had evidence of a known or suspected infection at study entry. Patients were randomized to placebo vs rosuvastatin 40 mg at the time of enrollment followed by 20 mg daily until the third day after intensive care unit discharge, study day 28, hospital discharge, or death. Rosuvastatin dose was reduced to 10 mg for patients with creatinine level ≥2.8 mg/dL (while not on dialysis). The primary predictor for the current analysis is rosuvastatin treatment as specified in the original trial in an intention-to-treat design.

The institutional review boards at each participating institution reviewed and approved the study protocol; informed consent was obtained from all patients or their health care surrogates.

Main Analysis

For the present analysis, we excluded 15 patients who were on chronic dialysis prior to the study and 86 patients with a missing creatinine measurement in the first 7 days after randomization. The remaining population was divided into those without AKI at the time of randomization and those with preexisting AKI at the time of randomization. AKI was defined using the Kidney Disease Improving Global Outcomes (KDIGO) creatinine-based criteria.¹⁰ The primary outcome for those without AKI at randomization was the development of de novo AKI within 7 days after randomization. De novo AKI is defined as an increase in creatinine by ≥0.3 mg/dL within 48 hours or an increase of creatinine by ≥50% from baseline over the first 7 days (with baseline creatinine defined as the lowest creatinine within 96 hours prior to randomization). The primary outcome for those with preexisting stage 1 AKI was the development of worsening (stage 2 or 3) AKI stage, including receipt of dialysis. Participants with preexisting stage 2/3 AKI were not included in regression analyses. Figure 1 illustrates the derivation of our analytic cohort.

Figure 1.

Screening, randomization, and derivation of analytic cohort.

We used multivariable logistic regression to determine the association between rosuvastatin and AKI outcomes. We a priori decided to adjust for age, sex, race, ethnicity, ARDS etiology (primary respiratory defined as pneumonia or aspiration, vs nonrespiratory etiology), and severity of illness defined using Acute Physiology, Age, Chronic Health Evaluation (APACHE) III scores.

We additionally performed exploratory analysis comparing peak serum creatine kinase (CK) levels between rosuvastatin and control groups, separately for those with and without preexisting AKI. The incidence of serum CK levels above 10 times the upper limit of normal were also compared between rosuvastatin and control groups, to mirror analysis performed in the original SAILS publication.⁸

All data were prospectively collected during the original trial. Analysis was conducted using STATA 14.1/SE (College Station, Texas).

Fluid-Adjusted Analysis

Prior data from the ARDS Network have shown that fluid balance can confound AKI ascertainment.¹¹ Correction of creatinine for fluid balance may reassign patients from AKI to non-AKI groups and vice versa. Therefore, we replicated previously published methodology^11,12 to adjust serum creatinine for volume of distribution. We first estimated the volume of distribution for creatinine on the day of randomization as the total body water (TBW), equaling 60% of body weight on randomization.¹³ We then calculated the on-study cumulative fluid balance using 24-hour fluid intake/output recorded. The final fluid-adjusted creatinine¹¹ is equal to the measured creatinine × (1 + [on-study cumulative fluid balance/TBW]). Patients are then reclassified as AKI or no AKI using fluid-adjusted creatinines, and the primary analysis was repeated using these fluid-adjusted values.

Results

Among 644 participants in our analytic cohort, 511 (79%) had no AKI, 93 (14%) had stage 1 AKI, and 40 (6%) had stage 2 or stage 3 AKI before randomization (Figure 1). Our cohort had similar characteristics as the original trial participants (Table 1). The median age was 55 (interquartile range [IQR]: 42-66), 51% were female, 14% were African American, and 12% were of Hispanic ethnicity. Mean baseline creatinine for both rosuvastatin and placebo groups were 1.2 mg/dL.

Table 1.

Baseline Characteristics of Study Participants.

Prerandomization characteristics	All (n = 644)	Placebo (n = 315)	Rosuvastatin (n = 329)	P
Age	54.2 (16.4)	54.1 (15.8)	54.4 (17.0)	.82
Median (IQR)	55 (42-66)	55 (43-65)	55 (42-67)
Female	329 (51%)	164 (52%)	165 (50%)	.63
Race				.68
White	515 (80%)	254 (81%)	261 (79%)
African American	88 (14%)	42 (13%)	46 (14%)
Other	20 (3%)	10 (3%)	10 (3%)
Unknown	21 (3%)	9 (3%)	12 (4%)
Hispanic ethnicity	76 (12%)	34 (11%)	42 (13%)	.77
Weight (kg)	87.7 (30.9)	86.6 (31.3)	88.8 (30.5)	.39
Median (IQR)	82 (68-100)	80 (66-100)	84 (69-100)
ARDS etiology
Direct (pneumonia or aspiration)	509 (79%)	247 (78%)	262 (80%)	.43
APACHE III score (n = 613)	93.2 (27.8)	94.7 (27.1)	91.7 (28.4)	.18
Baseline creatinine (mg/dL) (n = 640)	1.2 (0.9)	1.2 (0.9)	1.2 (0.9)	.62
Median (IQR)	0.9 (0.7-1.4)	1.0 (0.6-1.5)	0.9 (0.7-1.4)
AKI before randomization	133 (20%)	58 (18%)	75 (23%)	.17
AKI requiring dialysis	37 (6%)	20 (6%)	17 (5%)	.52

Note. IQR = interquartile range; ARDS = acute respiratory distress syndrome; AKI = acute kidney injury

Effect of Rosuvastatin on De Novo AKI

Among the 511 participants without preexisting AKI at randomization, 200 (39%) developed stage 1 or greater AKI after randomization. There were no significant differences in risk of AKI between the rosuvastatin and control groups. Further analysis using fluid-adjusted creatinines to ascertain AKI also showed no difference in AKI risk between the rosuvastatin and control groups (Table 2).

Table 2.

Effect of Rosuvastatin on Acute Kidney Injury Outcomes.

Outcome: de novo AKI in patients without preexisting AKI (n = 511)	Placebo (n = 257)	Rosuvastatin (n = 254)	P
Developed AKI	103 (40%)	97 (38%)	.66
Stage 1 (% out of all AKI)	44 (42.7%)	34 (35.1%)
Stage 2	11 (10.7%)	12 (12.4%)
Stage 3 without dialysis	32 (31.1%)	35 (36.1%)
Stage 3 with dialysis	16 (15.5%)	16 (16.5%)
Logistic regression analysis		OR (95% CI)
Crude	Reference	0.92 (0.65-1.32)	.66
Multivariable^a	Reference	0.99 (0.67-1.44)	.94
Fluid-adjusted analysis		OR (95% CI)
Crude	Reference	0.84 (0.59-1.21)	.35
Multivariable^a	Reference	0.92 (0.63-1.34)	.64
Outcome: worsened AKI in patients with preexisting stage 1 AKI (n = 93)	Placebo (n = 39)	Rosuvastatin (n = 54)	P
Developed ≥ stage 2 AKI post randomization	16 (41%)	33 (61%)	.06
Logistic regression analysis		OR (95% CI)
Crude	Reference	2.26 (0.97-5.24)	.06
Multivariable^a	Reference	3.06 (1.14-8.22)	.03
Fluid-adjusted analysis		OR (95% CI)
Crude	Reference	1.41 (0.61-3.27)	.42
Multivariable^a	Reference	1.85 (0.70-4.84)	.21

Note. AKI = acute kidney injury; OR = odds ratio; CI = confidence interval.

Multivariable analyses were adjusted for age, sex, race, ethnicity, ARDS etiology (primary respiratory etiology defined as either pneumonia or aspiration, vs nonrespiratory etiology), and severity of illness defined by APACHE III scores.

Effect of Rosuvastatin on Preexisting Stage 1 AKI

Among the 93 participants with preexisting stage 1 AKI at randomization, 49 (53%) progressed to stage 2 or higher AKI after randomization (Table 2). In our primary analysis, the rosuvastatin group had a 3-fold higher adjusted odds of worsening AKI (P = .03). However, this association was no longer significant in our secondary analysis when creatinine levels were adjusted for fluid balance (adjusted odds ratio: 1.85, 95% confidence interval [CI]: 0.70-4.84, P = .21). We found that there was a trend toward higher prevalence of vasopressor use before randomization in the placebo group (81%) compared with the rosuvastatin group (62%, P = .06) which was associated with higher mean fluid balance at randomization (+ 4.3 L in the placebo group vs + 2.5 L in the rosuvastatin group, P = .02).

Serum CK Levels

Table 3 shows the baseline and peak serum CK levels by subgroups and by placebo vs rosuvastatin treatment. Notably, among patients with preexisting stage 1 AKI at randomization, there was higher crude incidence of peak CK above 10 times the upper limit of normal for those treated with rosuvastatin (20%) vs those treated with placebo (8%; P = .09).

Table 3.

Serum CK Levels.

Subgroup without preexisting AKI at randomization (n = 511)	Placebo (n = 257)	Rosuvastatin (n = 254)	P
Baseline CK^a	201 ± 291	212 ± 405	.73
Peak CK^a	477 ± 1463	1070 ± 10141	.33
Peak CK > 10 times upper limit of normal	11 (4.3%)	15 (5.9%)	.40
Subgroup with preexisting stage 1 AKI at randomization (n = 93)	Placebo (n = 39)	Rosuvastatin (n = 54)	P
Baseline CK^a	389 ± 918	237 ± 566	0.33
Peak CK^a	754 ± 1676	3119 ± 15,474	0.35
Peak CK > 10 times upper limit of normal	3 (8%)	11 (20%)	0.09

Note. CK = creatine kinase.

Expressed as mean ± standard deviation, in U/L.

Discussion

In this analysis of patients with sepsis-associated ARDS enrolled in a randomized clinical trial, we found that rosuvastatin treatment did not protect against de novo AKI or worsening of existing mild AKI. To our knowledge, this is the first study to examine the effect of statin therapy in sepsis-associated AKI in humans. Our study adds to an emerging body of literature exploring whether statins may offer a renoprotective benefits.

Statins are potent lipid-lowering agents that are effective in preventing and treating coronary artery disease. The potentially nephroprotective effect of statin therapy is rooted in the “pleiotropic” effects including enhancement of nitric oxide production along with anti-inflammatory and antioxidant properties.¹⁴ Yet the benefits of statins on kidney disease remain controversial. A recent meta-analysis of more than 50 randomized controlled trials (RCTs) in which statins were given for at least 6 months concluded that statin therapy did not reduce the risk for kidney failure events (defined as end-stage renal disease, doubling of serum creatinine, or >25% or 50% decrease in estimated glomerular filtration rate [eGFR] depending on the study) among adults not already receiving dialysis, but that statin therapy may modestly reduce proteinuria and rate of eGFR decline.¹⁵

The potential role of short-term statin administration on AKI prevention has been investigated more recently in human studies. Several recent RCTs found that short-term precontrast statin administration may be protective against contrast-associated AKI (CA-AKI).^6,16-18 The largest of these studies randomized nearly 3000 patients in China with type 2 diabetes or mild to moderate chronic kidney disease undergoing coronary or peripheral arterial angiography to a 5-day course of rosuvastatin vs no statin and found the incidence of CA-AKI to be significantly lower in the rosuvastatin group (2.3% vs 3.9%, P = .01).¹⁶ However, more studies are needed to replicate the effect sizes seen in recent studies and to determine the best groups to target for CA-AKI. In the cardiac surgery setting, recent large RCTs found that statin administration did not protect against postoperative AKI,^7,19 while a possibility of renal harm was suggested by some data.^7,20

Our analysis did not demonstrate any renal benefit with rosuvastatin in patients with sepsis and ARDS. Rather, our primary analysis showed that rosuvastatin treatment may in fact be harmful in patients with preexisting AKI, though this finding may be confounded by prerandomization differences in fluid balance and vasopressor use between the groups. We had only a modest number of patients with preexisting AKI at randomization, which limited our power to detect potential harm or benefit. In the original SAILS study, enrollment was stopped early due to futility after 745 participants (out of planned 1000) for lack of benefit with regard to in-hospital mortality.⁸ Interestingly, in the original SAILS study, the rosuvastatin group had slightly fewer days free of renal failure (mean 10.1 days in the rosuvastatin arm vs 11.0 days in placebo arm, P = .01).⁸ However, renal failure was defined fairly crudely as serum creatinine level of at least 2.0 mg/dL in the original study, while our current analysis used a more updated consensus definition of AKI and incorporated both de novo AKI as well as worsening serum creatinine in those with preexisting AKI as outcomes. Therefore, we believe that a potentially detrimental renal effect of rosuvastatin—in the setting of sepsis—cannot be ruled out.

The mechanism for possible deleterious renal effect of statins is unclear. As the kidneys are responsible for excreting 10% of rosuvastatin (vs 90% eliminated in feces),²¹ it is plausible that patients with preexisting AKI were at higher risk of any potentially nephrotoxic effect due to higher circulating levels of rosuvastatin. AKI associated with statin administration is most commonly caused by rhabdomyolysis leading to acute tubular necrosis (often in the setting of concurrent use of fibrates or other interacting medications, which were exclusion criteria in the original SAILS study). Interestingly, in our exploratory analysis examining serum CK levels, we found higher peak CK levels in those treated with rosuvastatin compared with placebo, though these differences did not reach statistical significance. Among those with preexisting stage 1 AKI at randomization, rosuvastatin treatment is crudely associated with a nearly 3-fold increased odds of having peak CK above 10 times upper limit of normal, though this association again did not reach statistical significance, likely owing to the small sample of patients with preexisting AKI available for analysis. Based on our data, we cannot definitively conclude, nor rule out, that rhabdomyolysis (or subclinical levels of rhabdomyolysis) played a role in the association between rosuvastatin and worsening of AKI. There is indeed additional recent literature suggesting acute nephrotoxicity associated with high-potency statins,^22,23 with one case report of suspected direct tubular toxicity associated with high-dose rosuvastatin.²²

Our study has the following limitations. First, we did not use urine output to define AKI,²⁴ and creatinine measurements were not obtained daily for the entire 28-day treatment period. Second, no prehospitalization serum creatinine values were available. However, as part of the study protocol, all creatinine values from the 96 hours prior to randomization were systematically collected, and we used the lowest creatinine in the prerandomization period as reference. In addition, our current analysis may have been underpowered to detect significant differences in AKI outcomes, given our fixed sample size from the original SAILS trial. For example, we had an 80% power to detect a 12% difference in rate of de novo AKI among the 511 patients without preexisting AKI, and therefore a smaller effect size of rosuvastatin on AKI risk would not have been identified. Finally, given the requirement for sepsis-associated ARDS, the SAILS participants are critically ill with a mean APACHE III score of 93. Therefore, the results here may not be generalizable to all cases of sepsis-induced AKI. Nevertheless, this study is strengthened by randomized and protocoled exposure to rosuvastatin, and its completeness of prospectively collected data including severity of illness, fluid balance, vasopressor use, and preenrollment creatinine values. We also performed a thorough analysis adjusting serum creatinine for cumulative fluid balance, as fluid overload is common in this population and is known to influence AKI ascertainment.

Conclusions

In conclusion, we demonstrated that rosuvastatin treatment in critically ill patients with sepsis and ARDS did not prevent de novo AKI and did not prevent worsening of AKI in those with preexisting mild AKI. While statins have been proposed to be renoprotective in other settings, our study showed no renal benefit in sepsis-associated AKI, and potential harm of statin administration on exacerbating preexisting mild AKI cannot be ruled out.

Footnotes

Ethics Approval and Consent to Participate

Institutional Review Boards at each participating institution reviewed and approved the study protocol; informed consent was obtained from all patients or their health care surrogates.

Consent for Publication

All authors consent for publication.

Availability of Data and Materials

No.

Declaration of Conflicting Interests

The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Funding

The author(s) disclosed receipt of the following financial support for the research, authorship, and/or publication of this article: The original SAILS study was supported by a grant from the National Heart, Lung, and Blood Institute (NHLBI) (HHSN268200 536165C-536179C), and the Investigator-Sponsored Study Program of AstraZeneca. R.K.H. was supported by grants from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) (K23DK100468, R03DK111881). K.D.L. was supported by a grant from the NIDDK (K24DK113381). The funding sources had no role in the study design, study conduct, data analysis, or data interpretation.

ORCID iD

Raymond K. Hsu

References

Uchino

Kellum

Bellomo

et al . Acute renal failure in critically ill patients: a multinational, multicenter study. JAMA. 2005;294:813-818. doi:10.1001/jama.294.7.813.

Hoste

Bagshaw

Bellomo

et al . Epidemiology of acute kidney injury in critically ill patients: the multinational AKI-EPI study. Intensive Care Med. 2015;41(8):1411-1423. doi:10.1007/s00134-015-3934-7.

Yasuda

Yuen

Zhou

Star

RA.

Simvastatin improves sepsis-induced mortality and acute kidney injury via renal vascular effects. Kidney Int. 2006;69:1535-1542. doi:10.1038/sj.ki.5000300.

Yoshida

Yamashita

Iwai

Hayashi

Endothelial Krüppel-like factor 4 mediates the protective effect of statins against ischemic AKI. J Am Soc Nephrol. 2016;27:1379-1388. doi:10.1681/ASN.2015040460.

Gueler

Rong

Park

et al . Postischemic acute renal failure is reduced by short-term statin treatment in a rat model. J Am Soc Nephrol. 2002;13:2288-2298.

Ukaigwe

Karmacharya

Mahmood

et al . Meta-analysis on efficacy of statins for prevention of contrast-induced acute kidney injury in patients undergoing coronary angiography. Am J Cardiol. 2014;114:1295-1302. doi:10.1016/j.amjcard.2014.07.059.

Billings

Hendricks

Schildcrout

et al . High-dose perioperative atorvastatin and acute kidney injury following cardiac surgery: a randomized clinical trial. JAMA. 2016;315:877-888. doi:10.1001/jama.2016.0548.

Truwit

Bernard

Steingrub

et al . Rosuvastatin for sepsis-associated acute respiratory distress syndrome. N Engl J Med. 2014;370:2191-2200. doi:10.1056/NEJMoa1401520.

Bernard

Artigas

Brigham

et al . The American-European Consensus Conference on ARDS. Definitions, mechanisms, relevant outcomes, and clinical trial coordination. Am J Respir Crit Care Med. 1994;149:818-824. doi:10.1164/ajrccm.149.3.7509706.

10.

Kidney Disease: Improving Global Outcomes (KDIGO) Acute Kidney Injury Work Group. KDIGO clinical practice guideline for acute kidney injury. Kidney int. 2012;2(suppl):1-138.

11.

Liu

Thompson

Ancukiewicz

et al . Acute kidney injury in patients with acute lung injury: impact of fluid accumulation on classification of acute kidney injury and associated outcomes. Crit Care Med. 2011;39:2665-2671. doi:10.1097/CCM.0b013e318228234b.

12.

Grissom

Hirshberg

Dickerson

et al . Fluid management with a simplified conservative protocol for the acute respiratory distress syndrome. Crit Care Med. 2015;43:288-295. doi:10.1097/CCM.0000000000000715.

13.

Macedo

Bouchard

Soroko

et al . Fluid accumulation, recognition and staging of acute kidney injury in critically-ill patients. Crit Care. 2010;14:R82. doi:10.1186/cc9004.

14.

Yoshida

Hayashi

Pleiotropic effects of statins on acute kidney injury: involvement of Krüppel-like factor 4. Clin Exp Nephrol. 2016;21:175-181. doi:10.1007/s10157-016-1286-4.

15.

Zhang

et al . Effect of statins on kidney disease outcomes: a systematic review and meta-analysis. Am J Kidney Dis. 2016;67:881-892. doi:10.1053/j.ajkd.2016.01.016.

16.

Han

Zhu

Han

et al . Short-term rosuvastatin therapy for prevention of contrast-induced acute kidney injury in patients with diabetes and chronic kidney disease. J Am Coll Cardiol. 2014;63:62-70. doi:10.1016/j.jacc.2013.09.017.

17.

Leoncini

Toso

Maioli

Tropeano

Villani

Bellandi

Early high-dose rosuvastatin for contrast-induced nephropathy prevention in acute coronary syndrome: results from the PRATO-ACS Study (Protective Effect of Rosuvastatin and Antiplatelet Therapy On contrast-induced acute kidney injury and myocardial damage in patients with Acute Coronary Syndrome). J Am Coll Cardiol. 2014;63:71-79. doi:10.1016/j.jacc.2013.04.105.

18.

Quintavalle

Fiore

De Micco

et al . Impact of a high loading dose of atorvastatin on contrast-induced acute kidney injury. Circulation. 2012;126. 3008-3016. doi:10.1161/CIRCULATIONAHA.112.103317.

19.

Park

Shim

Song

Soh

Kwak

YL.

Effect of atorvastatin on the incidence of acute kidney injury following valvular heart surgery: a randomized, placebo-controlled trial. Intensive Care Med. 2016;42:1398-1407. doi:10.1007/s00134-016-4358-8.

20.

Zheng

Jayaram

Jiang

et al . Perioperative rosuvastatin in cardiac surgery. N Engl J Med. 2016;374:1744-1753. doi:10.1056/NEJMoa1507750.

21.

Luvai

Mbagaya

Hall

Barth

JH.

Rosuvastatin: a review of the pharmacology and clinical effectiveness in cardiovascular disease. Clin Med Insights Cardiol. 2012;6:17-33. doi:10.4137/CMC.S4324.

22.

Ward

John

Bargman

McQuillan

RF.

Renal tubular toxicity associated with rosuvastatin therapy. Am J Kidney Dis. 2017;69:473-476. doi:10.1053/j.ajkd.2016.08.037.

23.

Dormuth

Hemmelgarn

Paterson

et al . Use of high potency statins and rates of admission for acute kidney injury: multicenter, retrospective observational analysis of administrative databases. BMJ. 2013;346:f880.

24.

Md Ralib

Pickering

Shaw

Endre

ZH.

The urine output definition of acute kidney injury is too liberal. Crit Care. 2013;17:R112. doi:10.1186/cc12784.

Effect of Rosuvastatin on Acute Kidney Injury in Sepsis-Associated Acute Respiratory Distress Syndrome