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Severe acute kidney injury in critically ill COVID-19 patients

Journal of Nephrology volume 34pages 285–293 (2021)Cite this article

Abstract

Background

Acute kidney injury (AKI) is frequent in Coronavirus Infection Disease 2019 (COVID-19) patients. Factors associated with AKI in COVID-19 intensive care unit (ICU) patients and their outcomes have not been previously explored.

Methods

Prospective observational study of COVID-19 patients admitted to the ICUs of the Hospital Clínic of Barcelona (Spain), from March 25th to April 21st, 2020, who developed AKI stage 2 or higher (AKIN classification). The primary goal was to describe the characteristics of moderate-severe AKI of COVID-19 patients in an ICU context. As a secondary goal, we aimed to find independent predictors of AKI progression, Renal Replacement Therapy (RRT) requirement and mortality among these patients.

Results

During the study period, 52 out of 237 ICU patients, developed AKIN stage 2 or higher and were included in the study. A Sequential Organ Failure Assessment (SOFA) score at AKI diagnosis of 8 or higher was associated with RRT, OR 5.2, p 0.032. At the time of AKI diagnosis, patients had a worse liver profile and higher inflammation markers than at admission. Fifty per cent of the patients presented AKI progression from AKIN 2 to 3 and 28.85% required RRT. The use of corticosteroids in 69.2% of patients was associated with a reduced requirement of RRT, OR 0.13 (CI 95% 0.02–0.89), p 0.037. AKI was associated with high mortality (50%) and a longer hospital stay, median 35 vs 18 days (p 0.024).

Conclusions

The prevalence of moderate/severe AKI in COVID-19 patients admitted to the ICU is high and has a strong correlation with mortality and length of hospital stay.

Introduction

The outbreak of the new Coronavirus Infection Disease 2019 (COVID-19) has rapidly evolved into a global pandemic with devastating consequences [1, 2]. On May 20th, 2020, Spain had 232,555 patients affected by COVID-19 and ranked 5th in the world for most positive cases [3]. At the Hospital Clínic of Barcelona, the first case was detected on February 25th, and from then until May 21st, 2,418 patients were admitted to the institution, of whom, 444 (18.36%) required intensive care unit (ICU) admission.

COVID-19 patients predominantly develop respiratory symptoms, and in some patients, it evolves to acute respiratory distress syndrome (ARDS) or multi-organ failure, including kidney injury [3]. Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infects the host using the angiotensin-converting enzyme 2 receptor (ACE2) that is expressed in several organs, including the kidney [4,5,6,7]. Acute kidney injury (AKI) is frequent in COVID-19; reports from China, Italy, and the USA found a rate of AKI that ranges widely from 0.5 to 36.6% in hospitalized patients, and it portends poor prognosis [8,9,10,11,12,13,14,15,16]. As for critically ill patients, the described incidence was 19–23% [17, 18].

Several contributors have been proposed in the pathogenesis of AKI in patients with COVID-19: immunologic injury associated with inflammatory response, direct cytotoxicity over endothelial and tubuloepithelial cells and podocytes, microthrombi and thrombotic microangiopathy, or cardiorenal syndrome due to right ventricular failure may be present [19, 20].

Factors associated with AKI in COVID-19 ICU patients and their outcomes have not been previously explored. The objective of our study is to describe the characteristics of moderate-severe AKI in the ICU context. As a secondary objective, we attempted to find independent predictors of AKI progression to renal replacement therapy (RRT) requirement and mortality.

Methods

This is a prospective observational study. SARS-CoV-2 infection was diagnosed by reverse transcription-quantitative PCR (RT-PCR) assay of nasopharyngeal swab specimens. We included all the patients with COVID-19 who developed AKI ≥ 2 according to AKIN classification [21], and who were admitted to the ICUs of the Hospital Clínic of Barcelona (Spain) from March 25th to April 21st, 2020. The exclusion criteria were: chronic dialysis treatment, kidney transplant, or chronic kidney disease (CKD) KDIGO stage 4 (estimated glomerular filtrate rate (eGFR) less than 30 ml/min) [22]. The patients were followed-up until discharge from hospital, death, or the last follow-up day (July 15th, 2020).

Demographic variables, including Body Mass Index (BMI), date of illness onset and symptoms, vital signs, blood test studies and Sequential Organ Failure Assessment (SOFA) score (at hospital admission, at AKI stage 2 diagnosis, and at RRT start), use of vasoactive drugs, pharmacological treatments received, use of mechanical ventilation, RRT characteristics, urinary output at AKI stage 2, date of RRT start, date of ICU/hospital discharge and mortality were recorded. Comorbidities, which included cardiovascular disease, current or previous history of smoking, hypertension, diabetes, chronic obstructive pulmonary disease (COPD), human immunodeficiency virus (HIV) infection, and presence of active neoplasm, were also assessed, as were angiotensin-converting enzyme inhibitor (ACEI) and angiotensin receptor blocker (ARB) treatment at baseline. The suspected cause of AKI was evaluated; COVID-19-related AKI was considered if no other explanation was evident or suspected after diagnostic workup. RRT indication, modality and dose were based on clinical judgment.

In general, patients with hemodynamic stability and use of vasopressors at a dose lower than 0.1 mcg/kg/min received intermittent hemodialysis, according to our protocol. The choice between continuous hemodialysis with medium cutoff or continuous hemodiafiltration was based on logistic criteria and the experience of each intensive care unit within the hospital.

AKI recovery was defined if last creatinine level was less than twice that at baseline.

Overall mortality and length of stay (LOS) among patients with COVID-19 diagnosis admitted to the ICU during the study period, and without exclusion criteria, were collected and compared with the cohort of patients with AKI.

Statistical analysis

Data were described as mean ± standard deviation (SD) if normally distributed, or median and interquartile range otherwise. Categorical variables were expressed as absolute and relative (%) frequencies. Group comparisons were made by Student's t test, Logistic regression, Fisher's exact t test or Mann–Whitney U test for independent groups when appropriate. Statistical associations were explored univariately, and all p values < 0.05 were included in the multivariate analysis. Statistical analyses were performed using IBM SPSS statistics V25.0 software (IBM Corp, Armonk, NY, USA). A two-sided p value ≤ 0.05 was used to indicate statistical significance.

Results

General characteristics

Two-hundred and thirty-seven patients with COVID-19 and without exclusion criteria required ICU admission. Fifty-two (21.4%) patients presented AKI ≥ 2 of the AKIN classification and were included in the study. The median follow-up was 35.5 (IQR 36.75) days. Table 1 summarizes the demographic and clinical characteristics of the patients at hospital admission.

Table 1 Baseline characteristics of patients at hospital admission
Full size table

Patients were mostly male (76.9%), with a median age of 71.5 (61–74.75) years. Regarding comorbidities, 73.08% of the patients presented at least one, with hypertension, diabetes and COPD being the most frequent (59.6%, 21.2% and 21.2%, respectively). Overweight was present in 17% of the patients, and 13.5% presented CKD stage 3. Twenty-one per cent of the patients (n = 11) were on treatment with ACEI, and 15.4% with ARBs at admission. Both antihypertensive drugs were discontinued in all patients at admission.

The median time from symptom onset to hospital and ICU admission were 7 (IQR 5) and 10 (IQR 4) days, respectively. Pneumonia was present in 94.2% of cases, with a mean PaO2/FiO2 of 243 ± 155 mmHg, and a mean SOFA at admission of 5.78 ± 3.26.

Table 2 summarizes the laboratory findings. At the time of AKI diagnosis, patients had a worse liver profile, higher levels of d-dimer, procalcitonin, leukocytes, and platelets than at admission. C-Reactive Protein (CRP) levels were lower at AKI diagnosis compared to admission values. SOFA scores also showed a significant increase between admission and AKI diagnosis (5.79 ± 3.26 and 8.38 ± 2.43, respectively, p < 0.01).

Table 2 Laboratory findings
Full size table

Thrombotic events occurred in ten patients (19.23%): eight pulmonary thromboembolisms and two peripheral arterial occlusions. On the other hand, hemorrhagic complications occurred in 11 patients (21.15%): four gastro-intestinal bleeds, three retroperitoneal bleeds, three muscle and one central nervous system bleeds.

Treatment

Most of the patients received therapy with the combination of hydroxychloroquine, azithromycin (96.2%), and lopinavir/ritonavir (94.2%). Steroids were administered to 69.2% of the patients with a mean cumulative dose of 544 ± 496.38 mg of prednisone. Tocilizumab was used in 48.1% of cases; the median time between admission and tocilizumab administration was two days (1–4), mean dose 561 ± 276.24. Five (9.6%) patients with refractory inflammatory response were treated with Anakinra.

Regarding antithrombotic treatment, 5 (9.6%) patients were anticoagulated, 38 (73%) received antithrombotic prophylaxis, and 9 (17.3%) did not receive antithrombotic therapy at hospital admission. At diagnosis of AKI, 10 (19.2%) patients were on anticoagulant treatment, 38 (73%) with prophylaxis and 4 (7.7%) without antithrombotic therapy. Low molecular weight heparin was used in 40 (76.9%) and 43 (82.69%) patients at admission and at AKI diagnosis, respectively. Moreover, three and five patients received unfractionated heparin at hospital admission and AKI diagnosis, respectively. One patient received fondaparinux at AKI time because of heparin-induced thrombocytopenia.

AKI characteristics

AKI characteristics and evolution are described in Table 3. Most of the patients (84.6%) developed AKI during the ICU stay, within a median of 5 and 12 days from admission and the onset of symptoms, respectively. Twenty-six (50%) of the cases progressed to more severe AKI.

Table 3 AKI characteristics and evolution of the patients
Full size table

Patients were mostly non-oliguric at AKI diagnosis, but those who started RRT developed it more frequently (in the 24 h before RRT onset). Hyperkalemia was not a frequent finding at the time of AKI diagnosis.

At AKI diagnosis, 73% of the patients were on treatment with vasoactive drugs, with a median noradrenaline dose of 0.19 mcg/kg/min (IQR 0.46).

Suspected intrinsic AKI related to severe COVID-19, which accounted for 71.15% (n 37) of cases, was the most common form of kidney dysfunction. The other probable causes of AKI that were identified included: hemorrhagic shock related to anticoagulation treatment (4); contrast nephropathy (3); drug nephrotoxicity (2); cardiac arrest (2); liver failure (2); heart failure (1) and pancreatitis (1).

Fifteen patients (28.85%) required RRT, including 13 with continuous renal replacement therapy (CRRT). Median time from admission to RRT was 12 (IQR 10) days. RRT mean time was 10.87 ± 9.28 days. CRRT was the only modality in eight patients, while five patients received CRRT followed by intermittent modality, and two patients were treated with intermittent modalities alone. When CRRT was used, the modalities included continuous hemodialysis with medium cut-off dialyzers (MCO) (n = 5) and continuous hemodiafiltration with high-flux hemofilter (n = 8). Anticoagulation consisted of citrate in six patients and heparin in six patients.

At the end of follow-up, 31 (59.6%) patients recovered from the AKI episode.

Outcomes

Variables associated with RRT or mortality are described in Tables 4 and 5 and 6 (Supplementary material).

Table 4 Univariate and multivariate analysis of clinical characteristics and treatment related to RRT
Full size table
Table 5 Univariate and multivariate analysis of clinical characteristics and treatment related to in-hospital mortality
Full size table

Baseline and admission creatinine was higher in patients who died, p 0.011 and 0.02, respectively (Table 6 supplementary materials). In univariate analysis, the variables associated with higher mortality in AKI patients were age > 60 years (p 0.017), and presence of one or more comorbidities (p 0.03). On the contrary, recovery from AKI was associated with less probability of death, p < 0.001. In the multivariate analysis, only AKI recovery retains significance (p 0.005).

Overall mortality among patients with COVID-19 diagnosis admitted to the ICUs during the study period, and without exclusion criteria, n = 237, was 16.87% (n = 40). In the non-AKI patients, mortality was 7.3% (n = 13), while in AKI patients it was 51.92% (n = 27), p < 0.001, OR 10.67 (95% CI 5.1–22.33). The median time to death after AKI diagnosis was eight days (IQR 13). AKI was also associated with longer hospital LOS, 35 (IQR 36.75) vs 18 (IQR 20) days in AKI vs non-AKI patients, respectively (p 0.018)).

Regarding RRT, in the univariate analysis, a SOFA score of 8 or more at AKI diagnosis was associated with the need for RRT, p 0.032, OR 4.52, with sensitivity and specificity of 73% and 62%, respectively. However, the non-renal SOFA score at AKI was not associated with RRT. Also the use of vasoactive drugs at AKI diagnosis was not associated with RRT requirement, p 0.06. On the contrary, the use of corticosteroids was associated with less requirement of RRT, p 0.03, OR 0.24.

In the multivariate analysis, a SOFA score of 8 or more and corticosteroid use at AKI diagnosis were associated with RRT, OR 6.15, p 0.015, and OR 0.16, p = 0.017 respectively.

Discussion

Kidney involvement is frequent in COVID-19. Cheng et al. described kidney abnormalities in more than 40% of COVID-19 patients in Wuhan (China), including proteinuria, hematuria and elevated serum creatinine [14]. Also, any degree of AKI has been associated with mortality in COVID-19 hospitalized patients [9,10,11, 13,14,15, 17, 23]. In this prospective observational single-center study, moderate-severe AKI was associated with high mortality (50 vs 7.3%) and hospital length of stay (35 vs 18 days).

Several mechanisms of kidney damage have been described, but many facts point to direct damage. Low counts of SARS-CoV-2 virus have been detected in kidney cells [20]; furthermore, SARS-CoV-2 infects the host using the ACE2 receptor, transmembrane serine protease 2, and cathepsin L, all are enriched in kidney tissue [24]. Even more endothelial cells express ACE2 receptors, and direct infection of SARS-CoV-2 on engineered human blood vessel organoids has been described [25]. Kidney histology in patients with COVID-19 has shown the presence of acute tubular necrosis, and moderate-to-severe lymphocytic infiltration and collapsing glomerulopathy [12, 20, 26]. The virus could also initiate CD68 + macrophage infiltration together with complement C5b-9 deposition to mediate tubular damage [12].

In our cohort, AKI episodes occurred together with worsening respiratory symptoms (median time from admission to AKI of 5 days), which supports either a direct mechanism of damage to the kidney or an immune-mediated one. In this sense, patients had higher bilirubin, d-dimer, and platelets at AKI diagnosis compared to the admission levels, supporting the hypothesis that severe AKI is part of multiorgan failure that occurs in the context of the cytokine storm that has been described in these patients. In accordance with this, a SOFA score of 8 or more at the time of AKI diagnosis was associated with higher RRT requirement. Also, procalcitonin was higher at the time of AKI diagnosis, which could be related to an inadvertent bacterial co-infection. Bacterial over infection cannot be ruled out as a worsening factor in AKI patients. However, it was not possible to confirm this overlap beyond a suspected diagnosis in most patients.

The treatment protocol for COVID-19 in our center included antiviral therapy with lopinavir/ritonavir, hydroxychloroquine and azithromycin. If patients showed clinical deterioration then biological therapy, which in the majority of cases included an anti-IL-6 (tocilizumab), an anti-IL-1 (anakinra) and/or corticosteroids, was recommended. In our cohort, the inflammatory response was treated with corticosteroids and tocilizumab in 69.2% and 48.1% of cases, respectively, at a median time of two days after admission. The use of corticoids was associated with a 13% reduction in RRT requirement.

In our cohort, 19.23% of patients presented a thrombotic event, confirming the high incidence reported in the literature [15, 27, 28]. Antithrombotic prophylaxis or anticoagulation was initiated in most of the patients. It is possible that microthrombi and thrombotic microangiopathy can contribute to the pathogenesis of AKI in patients with COVID-19 [15], but given the low number of cases that did not receive these treatments in our study, associations with AKI outcome could not be established. Nevertheless, we want to emphasize the relatively high incidence of major bleeding complications (21.15%). Patients with impaired kidney function have an increased risk of bleeding, and therefore, the risk/benefit of thromboprophylaxis must be balanced.

The treatments used in our cohort may have altered the course of AKI as the number of patients who required RRT in the present study is relatively low (15/237, 6%) compared to other recent cohorts with an incidence of RRT in ICU patients between 17 and 51% [12, 13, 16, 17, 23, 29, 30].

The present study has some limitations. First, given the observational nature of the study, bias cannot be ruled out in the beneficial effect of the corticosteroids. Second, the limited number of patients with RRT makes it challenging to come to conclusions about the best strategy for dialyzing patients. Also, the usefulness of MCO in the COVID-19 cytokine release syndrome needs further investigation in randomized studies [12].

An important point to consider is that all the patients with CKD KDIGO stage 4 were excluded from the present study to more clearly demonstrate the impact and evolution of AKI in the context of severe COVID-19. Therefore, these results cannot be extrapolated for patients with severe chronic kidney disease.

Given the observational nature of the study, there are no details on proteinuria and hematuria since they were not generally evaluated in our center during the pandemic. There is also no histological material, which would be very useful to describe the type of injury in AKI associated with COVID-19.

In conclusion, in our study the prevalence of moderate/severe AKI in COVID-19 in the ICUs is associated with high mortality and hospital length of stay. Present data suggest that corticosteroid treatment may be related to less RRT, but further research is needed to confirm these data.

Code availability

Not applicable.

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Acknowledgements

The Collaborator names on behalf of the Hospital Clínic Critical Care COVID-19 working group (CCCC) are A. Almuedo, JR Alonso, R. Andrea, F. Aziz, JR. Badia, E. Barbeta, X. Borrat, E. Bragulat, I. Carmona, M. Castellà, P. Castro, O. De Diego, M. Farrero, J. Fernández, S. Fernández, C. Ferrando, M. Ferrer, M. Forga, E. Guasch, Mª Hernández-Tejero, A. Jacas, P. Leyes, T. López, JA. Martínez, G. Martínez-Palli, R. Mellado, J. Mercadal, G. Muñoz, J. Muñoz, R. Navarro, JM Nicolás, J. Ortiz, E. Poch, M. Pujol, E. Quintana, E. Reverter, I. Rovira, P. Ruiz, E. Sandoval, S. Schneider, F. Seguí, O. Sibila, C. A. Soriano, D. Soy, M. Suárez, A. Téllez, ND. Toapanta, A. Torres, X. Urra.

Funding

The authors received no financial support for the research, authorship, and/or publication of this article.

Author information

Author notes

  1. Gaston J. Piñeiro and Alicia Molina-Andújar equally contributed.

Affiliations

  1. Nephrology and Kidney Transplantation Department, Hospital Clínic, IDIBAPS, University of Barcelona and REDinREN, Villarroel 170, 08036, Barcelona, Spain

    Gaston J. Piñeiro, Alicia Molina-Andújar, Evelyn Hermida, Miquel Blasco, Luis F. Quintana & Esteban Poch

  2. Surgical Intensive Care Unit, Anesthesiology Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Guido Muñoz Rojas & Jordi Mercadal

  3. Intensive Care Unit, Internal Medicine Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Pedro Castro

  4. Cardiovascular Intensive Care Unit, Cardiovascular Surgery Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Elena Sandoval

  5. Acute Cardiac Care Unit, Cardiology Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Rut Andrea

  6. Intensive Care Unit, Hepatology Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Javier Fernández

  7. Respiratory Institute, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Joan Ramon Badia

  8. Infectious Diseases Department, Hospital Clínic, IDIBAPS, Univesitat de Barcelona, Barcelona, Spain

    Alex Soriano

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  1. Gaston J. Piñeiro
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  10. Rut Andrea
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  13. Alex Soriano
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Consortia

the Hospital Clínic Critical Care COVID-19 working group (CCCC)

  • A. Almuedo
  • , J. R. Alonso
  • , R. Andrea
  • , F. Aziz
  • , J. R. Badia
  • , E. Barbeta
  • , X. Borrat
  • , E. Bragulat
  • , I. Carmona
  • , M. Castellà
  • , P. Castro
  • , O. De Diego
  • , M. Farrero
  • , J. Fernández
  • , S. Fernández
  • , C. Ferrando
  • , M. Ferrer
  • , M. Forga
  • , E. Guasch
  • , M. Hernández-Tejero
  • , A. Jacas
  • , P. Leyes
  • , T. López
  • , J. A. Martínez
  • , G. Martínez-Palli
  • , R. Mellado
  • , J. Mercadal
  • , G. Muñoz
  • , J. Muñoz
  • , R. Navarro
  • , J. M. Nicolás
  • , J. Ortiz
  • , E. Poch
  • , M. Pujol
  • , E. Quintana
  • , E. Reverter
  • , I. Rovira
  • , P. Ruiz
  • , E. Sandoval
  • , S. Schneider
  • , F. Seguí
  • , O. Sibila
  • , C. A. Soriano
  • , D. Soy
  • , M. Suárez
  • , A. Téllez
  • , N. D. Toapanta
  • , A. Torres
  •  & X. Urra

Contributions

GP, AMA and EP contributed to the study conception and design. Material preparation, data collection and analysis were performed by GP, AMA, EH and MB. The first draft of the manuscript was written by GP and AM. MB, EH, LFQ, GMR, JM, PC, ES, RA, JF, JRB, AS, EP: interpreted the data, revised the manuscript, provided intellectual content and approved the final version.

Corresponding author

Correspondence to Gaston J. Piñeiro.

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The authors declare no conflict of interest.

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The datasets used and/or analyzed during the current study are available from the corresponding author on reasonable request.

Ethics approval

The Institutional Ethics Committee approved the study with the identification code HCB/2020/0569. Informed consent was obtained from the patients or their legal representative, in accordance with the regulations of the ethics committee for patients with COVID-19.

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The Collaborator names of the Hospital Clínic Critical Care COVID-19 working group (CCCC) is given in the Acknowledgements section.

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Piñeiro, G.J., Molina-Andújar, A., Hermida, E. et al. Severe acute kidney injury in critically ill COVID-19 patients. J Nephrol 34, 285–293 (2021). https://doi.org/10.1007/s40620-020-00918-7

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  • DOI: https://doi.org/10.1007/s40620-020-00918-7

Keywords

  • COVID-19
  • Acute kidney injury
  • Intensive care
  • Renal replacement therapy