key: cord-1005959-ypl6qyvp
authors: Ramires, Marina Larissa Vettorello; Leite, Manoela Fidelis Batista; Lo, Daniel Zu Yow; da Silveira, Leonardo Bonilla; Ferraz, Leonardo José Rolim; Pardini, Andreia; Sakashita, Araci Massami; Kondo, Andrea Tiemi; Olivato, Guilherme Benfatti; Durão, Marcelino de Souza; Rodrigues, Adelson Marçal; Chiloff, Daniela Mendes; de Almeida, Danilo Candido; Goes, Miguel Angelo
title: Relation between red blood cell distribution width and acute kidney injury in patients with sepsis
date: 2022-05-02
journal: Einstein
DOI: 10.31744/einstein_journal/2022ao6828
sha: bac36efc67def61f3273e22a8efdf65d89452643
doc_id: 1005959
cord_uid: ypl6qyvp

OBJECTIVE: The objective of the present study is to evaluate the association of red blood cell distribution width with acute kidney injury in sepsis. METHODS: This is a retrospective study of 849 critically ill patients with sepsis in intensive care unit. Demographic data, renal function, inflammation, complete blood count, and acid-base parameters were compared between acute kidney injury and non-acute kidney injury groups. Therefore, a multivariate analysis was performed to observe independent predictive factors. RESULTS: Comparatively, higher levels of C-reactive protein, lactate, red blood cell distribution width, and Simplified Acute Physiology Score 3 were found in the acute kidney injury group. The study showed a higher frequency of women, hemoglobin (Hgb) concentration, platelets, bicarbonate and PaO(2)/FiO(2) ratio in the non-acute kidney injury group. In addition, there was an independent association of comorbidity-chronic kidney disease [OR 3.549, 95%CI: 1.627-7.743; p<0.001], urea [OR 1.047, 95%CI: 1.036-1.058; p<0.001] and RDW [OR 1.158, 95%CI: 1.045-1.283; p=0.005] with acute kidney injury in sepsis patients. CONCLUSION: As an elective risk factor, red blood cell distribution width was independently associated with sepsis-related acute kidney injury. Thus, red blood cell distribution width acts like a predictive factor for sepsis-induced acute kidney injury in intensive care unit admission.

Acute kidney injury (AKI) is a common and serious syndrome with a high number of cases worldwide. Sepsis is the most important cause of AKI in critically ill patients with high mortality in the intensive care unit (ICU). (1) (2) (3) (4) Sepsis causes hypoperfusion with lower oxygenation and bicarbonate concentration but with higher lactate levels, with consequent organic dysfunction in critically ill patients admitted to the ICU. (2) (3) (4) (5) (6) In line with this, sepsis-associated AKI is complex and multifactorial. It includes endothelial and tubule changes, infiltration of inflammatory cells, and intrarenal hemodynamic changes with intraglomerular thrombosis. (3) (4) (5) (6) In addition, AKI in sepsis may also be distinguished from non-sepsis AKI by some specific features and poor prognosis. (2) einstein (São Paulo). 2022;20:1-7

Considering the hematological context, red cell distribution width (RDW) measures the amount of red blood cell variation in volume and size. The RDW is defined as the standard deviation of erythrocyte size divided by the mean corpuscular volume. (7) In some cases, changes in RDW indicates blood-associated abnormalities or organ/systems dysfunction and acts as a predictor of outcomes in critically ill patients. (8) (9) (10) (11) (12) In addition, RDW is a readily available biomarker related to decreased hemoglobin levels by inflammatory cytokines and impairing iron mobilization. (7) (8) (9) (10) Further, RDW can integrate various pathophysiological mechanisms associated with sepsis. (8, 9, (11) (12) (13) Recently, researchers have reported an independent association of RDW and the risk of adverse outcomes in patients with sepsis. (10, 11) However, no evidence of the RDW association with sepsis-induced AKI was found. Therefore, this study analyzed the relationship of RDW and sepsis-induced AKI.

❚ OBJECTIVE To analyze whether red blood cell distribution width could act as a predictor of acute kidney injury in patients with sepsis.

Medical records of patients with sepsis who were admitted to any unit of the Intensive Care Center of Hospital Israelita Albert Einstein (HIAE), São Paulo, Brazil, from January 1 to December 31, 2017, were retrospectively studied. First, the study observed that the patients were screened by quick Sequential [Sepsis-related Organ] Failure Assessment (qSOFA) for early suspected sepsis in the emergency department or bedside in the ward. A qSOFA ≥2 was considered altered with the following variables: Glasgow coma score <15, respiratory rate ≥22 breaths/minute, systolic blood pressure ≤100mmHg. (14) Afterward, the patient was referred to the ICU.

Inclusion criteria were individuals over 18 years of age with a diagnosis of sepsis admitted to an ICU at HIAE. Patients with hematologic, advanced oncological disease, liver failure, chronic infection by HIV, hepatitis B and C, chronic kidney disease (CKD) stages 4 or 5, and patients who died within the first 24 hours of admission to the ICU were excluded.

The variables analyzed were age, sex, Hgb concentration, blood count parameters such as mean corpuscular volume, RDW, platelet, white blood cell count, serum levels of urea, creatinine, sodium, potassium, total bilirubin, C-reactive protein (CRP), arterial blood gas parameters, arterial lactate, arterial oxygen pressure/inspired oxygen fraction (PaO 2 /FiO 2 ) ratio, and Simplified Acute Physiology Score 3 (SAPS 3) prognostic index. (15) Outcomes such as AKI, need for Renal Replacement Therapy (RRT), red cell transfusion, mechanical ventilation, vasopressor drugs, and mortality were computed. Norepinephrine was the primary vasopressor used when mean arterial pressure was maintained <65mmHg after volume resuscitation. Continuous venovenous hemodiafiltration was used in patients with hemodynamic instability, and intermittent hemodialysis was used in stable hemodynamic patients who required RRT during the ICU period.

Acute kidney injury was defined and stratified according to the Kidney Disease Improving Global Outcomes (KDIGO) criteria, if there was an increase of 0.3mg/dL in 48 hours, or a 1.5-fold increase in serum creatinine in seven days, or diuresis lower than <0.5mL/kg/hour during six hours from ICU admission. (16) A follow-up up to 28 days after admission to the ICU was conducted to determine the outcomes. This study was approved by the local ethics committee on human research at HIAE, São Paulo, Brazil (CAAE: 01520218.9.0000.0071; protocol: 3.025.097, CAAE: 02628918.7.0000.0071; protocol: 3.102.869 and CAAE: 93612218.2.0000.0071; protocol: 4.246.520). The study was conducted under the ethical standards of the responsible committee on human experimentation (institutional and national). Informed consent was waived, and researchers analyzed only not identified data.

Categorical variables are presented as frequencies and percentages. Numerical data were described as mean ± standard deviation. In a comparative analysis, the χ 2 test for frequencies was used. The Kolmogorov-Smirnov test was performed to find the normal distribution of continuous data. Afterward, the comparisons between the groups were made by the Student's t-test for data with normal distribution and Mann-Whitney for nonparametric data. The Pearson correlation between two continuous variables was also performed, in addition to the binary logistic regression with the backward stepwise method for admission data using AKI as a variable response. The variables in the multivariate model were included when reached p<0.09. Regression data were expressed as odds ratios (OR) and 95% confidence intervals (95%CI). Moreover, the association by regression of ICU admission markers with the need for RRT and mortality was also determined. For that analysis, the marker variables from ICU admission that einstein (São Paulo). 2022;20:1-7 were independently significant with AKI were used. The statistical level p<0.05 was considered significant. Statistical analyses were performed in SPSS version 22 (IBM, Armonk, New York, USA) and Excel TM 16.0 (Microsoft, Redmond, Washington, USA).

After exclusion criteria (Figure 1 ), the study was conducted with 849 patients with a diagnosis of sepsis. Classically, the patients were investigated about their primary site of infection. In these sepsis patients, 352 had respiratory tract infection, 183 had urinary tract infection, 139 had an undetermined primary focus, 105 had an abdominal infection, 50 had nervous system infection, and 20 patients had bloodstream infection as the focus of sepsis. Next, several admission variables of all patients were analyzed using multiple correlations. A positive correlation was found between age and SAPS 3 (r=0.57, p<0.001), SAPS 3 and RDW (r=0.35, p<0.001; Figure 2 ), RDW and urea (r=0.24, p<0.001), RDW and total bilirubin (r=0.24, p<0.001), RDW and age (r=0.21, p<0.001), RDW and lactate arterial (r=0.20, p<0.001), RDW and creatinine (r=0.18, p<0.001). Negative correlations were identified between bicarbonate and lactate concentration (r=-0.39, p<0.001), Hgb concentration and SAPS 3 (r=-0.34, p<0.001), Hgb and RDW (r=-0.32, p<0.001), bicarbonate and creatinine (r=-0.20, p<0.001), creatinine and Hgb (r=-0.16, p<0.001), and between Hgb and age (r=-0.15, p<0.001).

A positive correlation was found between simplified acute physiology score 3 and red blood cell distribution width in 849 patients with sepsis (p<0.001).

Furthermore, this study found that, among the total of sepsis patients, 294 had AKI diagnosis by KDIGO criteria. A total of 160 patients were in stage 1, 73 in stage 2, and 61 in stage 3, considering the KDIGO criteria. Thereafter, patients with sepsis were divided into two groups: AKI and without AKI (non-AKI) to perform several comparisons and associations. Table 1 shows that the AKI Group had a higher frequency of men and comorbidities (diabetes mellitus (DM), hypertension, and CKD) compared to the non-AKI Group. Lower indices for mean arterial pressure, Hgb concentration, platelets, pH, pCO 2 , arterial bicarbonate, and PaO 2 /FiO 2 ratio in AKI Group were found in comparison to non-AKI. Moreover, the AKI Group had higher mean age, and higher levels of creatinine, urea, total bilirubin, RDW (Figure 3 ), pO 2 , arterial lactate, and SAPS 3 prognostic index on admission to ICU compared to the non-AKI Group.

Higher red blood cell distribution width (%) at intensive care unit admission was found in sepsisinduced AKI Group compared to non-AKI Group (p<0.001).

In sequence with this analysis, table 2 showed that women and higher levels of bicarbonate have a protective effect against the risk of AKI associated with sepsis (around 65% and 12%, respectively). On the other hand, patients with higher levels of urea, RDW, and non-dialysis CKD at admission to the ICU are independently associated with AKI in sepsis. 

The main finding of the present study is that RDW is an independent predictor associated with AKI in critically ill patients with sepsis. In addition, the study identified that the highest RDW on admission was associated with the need for RRT during the ICU period.

The patients with sepsis-associated AKI had lower mean arterial pressure and arterial bicarbonate, but with elevated arterial lactate at admission, which symbolizes a situation according to low perfusion and organ dysfunction that often occurs in sepsis. (17, 18) Therefore, the relevance of the current study is corroborated by recent studies. (17, 19) Sepsis is the most important cause of AKI in the ICU and it is estimated that 15% to 20% of patients with sepsis-associated AKI need RRT. (17) When correlations were analyzed in patients with sepsis, negative associations of bicarbonate with both lactate and creatinine were identified. In addition, a positive correlation of RDW value with variables of poor renal function (urea and creatinine) was found.

The diagnosis of AKI is currently based on increased serum creatinine concentration and/or decreased urine output. (5, 16, 19, 20) Thus, the present study could define and form groups of patients with and without AKI. The group of patients who developed sepsisassociated AKI had lower PaO 2 /FiO 2 ratio, but higher levels of urea, creatinine, arterial lactate, RDW, and SAPS 3 prognostic index. All these clinical parameters indicate kidney dysfunction, decreased oxygenation, and lower tissue perfusion. Thus, there is more severity and poorer prognosis in patients with AKI associated with sepsis. On the one hand, this study group has recently demonstrated that critically ill patients with COVID-19-related AKI had a lower PaO 2 /FiO 2 ratio too. (21) Indeed, lung dysfunction from AKI is associated with poorer outcomes. (22) On the other hand, Loveday et al. reported the addition of RDW to APACHE III increased the prognostic value in critically ill patients. (9) Moreover, serum creatinine as a marker of renal function is a variable of the SAPS 3 prognostic index, reflecting greater levels of this prognostic index in patients with AKI. (9, 15) Furthermore, the current study found a positive correlation between the prognostic index-SAPS 3 and RDW. This indicates a relationship between RDW and prognostic index for critically ill patients. However, the present results corroborate with the results of other studies.

Moreover, the results of the present study were different from the results of Radovic et al., which observed levels of arterial lactate as an independent predictor of AKI but in patients undergoing cardiac surgery. (23) On the other hand, arterial lactate did not present an independent association with sepsisinduced AKI in the current study. Even so, this study found that the levels of bicarbonate on admission to the ICU were lower in the group that developed AKI. In addition, a multivariate analysis showed that higher levels of arterial bicarbonate have a protective effect on developing AKI. These findings agree with the results of Jung et al., who observed that low levels of serum bicarbonate were associated with a higher incidence of AKI and prolonged ICU stay after cardiac surgery. (24) The RDW is routinely reported as part of a complete blood cell count and expresses variation in the size of circulating erythrocytes. (7, 8, 12) Red cell distribution width is reported as a marker and predictive value in many clinical settings. Changes and disorders frequently seen in sepsis such as ineffective erythropoiesis or increased destruction of red blood cells cause anemia and consequently greater heterogeneity in the size of these cells and higher RDW. (7, 9, 10) Moreover, previous studies showed that RDW is associated with AKI in patients with traumatic brain injury, sepsis in pediatric patients, after cardiac surgery, and those with coronary disease. (25) (26) (27) (28) The present study confirmed the results found by other researchers. Moreover, as there were higher levels of CRP, arterial lactate, and RDW, in parallel with lower arterial bicarbonate, PaO 2 /FiO 2 ratio, platelets, and Hgb concentration in patients with sepsis and AKI, (7, 8, 17) it can be assumed that when inflammation occurs, it reduces iron metabolism, and bone marrow function is inhibited, thus, the erythrocyte proliferation and maturation are inhibited, (29, 30) leading to increased RDW einstein (São Paulo). 2022;20:1-7 values and anemia, (31) while inflammatory dysregulation can reduce tissue perfusion and thus cause AKI.

This study also found that RDW levels were higher in patients who developed AKI and showed that RDW at admission to ICU had an independent association with AKI in multivariate analysis. Interestingly, each 1% of the increase in the RDW value measured was independently associated with important risk (16%) of sepsis-induced AKI. Furthermore, each increase of 1mg/dL in the value of urea (higher than the cut-off of 50mg/dL) at admission was independently associated with a risk of 4% more of sepsis-associated AKI. The current study also found that female sex, and higher serum bicarbonate levels on admission to the ICU were associated with protection against sepsis-induced AKI.

Furthermore, it was also detected that the patients with CKD in stages 1-3, had 3.5 times more likely to develop AKI associated with sepsis independently. Other researchers reported a bilateral interaction of CKD with AKI. Chronic kidney disease predisposes to AKI. On the other hand, severe AKI could worsen the progression of CKD. (32) Even so, the present results showed a relationship between RDW and sepsis-associated AKI also in the subgroup of patients without CKD. Thus, eliminating the interference of CKD in this relationship.

Subsequently, the association of variables at ICU admission independently related to AKI with outcomes within 28 days was also analyzed. Each increase of 1mg/dL in the value of urea higher than the cut-off of 50mg/dL at ICU admission was associated with an increased risk (2.3%) of need for RRT. In turn, each 1% increase in the RDW value measured was associated with the risk (18%) of need for RRT. Also, there was association between mortality within 28 days of ICU stay and both urea and RDW value at ICU admission. Thus, each 1% increase in the measured RDW value was independently associated with 37% likely of mortality at 28 days of ICU stay. Thereby, these results are in robust compliance with other studies. In fact, Oh et al. reported that RDW is a predictor for all-cause mortality in AKI patients on RRT treatment in the ICU. (33) Fernandez et al. reported higher values of RDW as a marker of severity in patients discharged from the ICU. (34) Although intriguing, the present study has some potential limitations. First, the sample evaluated is from a retrospective cohort study. Second, it was in a singlecenter, there was no intervention by the researchers or sequential analysis of RDW, and there was no prespecified hypothesis. Finally, given the large number of potential predictors evaluated and the initial lack of selection guided by hypotheses of variables, the possibility of confounding bias cannot be ruled out.

Despite these limitations, one of the main strengths of this study is that it is based on routine blood tests for critically ill patients on admission to the ICU and is inexpensive. Thus, a strong and independent association of RDW with sepsis-induced AKI was found, reflecting severity and organ dysfunction. However, the present study showed that the RDW on ICU admission acts as a predictor of AKI associated with sepsis.

❚ CONCLUSION This study concluded that red cell distribution width can be used as a cost-effective marker for sepsis-associated acute kidney injury. Thus, further studies should be conducted to analyze the true predictive value of red blood cell distribution width in sepsis-induced acute kidney injury.

Anonymous and unidentified data are available upon reasonable request to the corresponding author and authorization by the research ethics committee.

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We thank all professionals and technicians from the intensive care unit of Hospital Israelita Albert Einstein, São Paulo, Brazil, for providing support in design, chart analysis and in manuscript review. A special thanks to the Nephrology Division, Universidade Federal de São Paulo, for their support and consideration.