Serum ferritin at admission in hospitalized COVID-19 patients as a predictor of mortality

Lino, Katia; Guimarães, Gabriel Macedo Costa; Alves, Lilian Santos; Oliveira, Any Caroline; Faustino, Renan; Fernandes, Cintia Souza; Tupinambá, Gleiser; Medeiros, Thalia; Silva, Andrea Alice da; Almeida, Jorge Reis

doi:10.1016/j.bjid.2021.101569

ABSTRACT

Introduction:

Some COVID-19 patients have higher mortality and the responsible factors for this unfavorable outcome is still not well understood.

Objective:

To study the association between ferritin levels at admission, representing an inflammatory state, and hospital mortality in COVID-19 patients.

Methods:

From May through July 2020, SARS-CoV-2 positive patients with moderate to severe clinical symptoms were evaluated at admission, regarding clinical and laboratory data on renal and hepatic function, hematologic parameters, cytomegalovirus co-infection, and acute phase proteins.

Results:

A total of 97 patients were included; mean age = 59.9 ± 16.3 years, 58.8% male, 57.7% non-white, in-hospital mortality = 45.4%. Age, ferritin, C-reactive protein, serum albumin and creatinine were significantly associated with mortality. Ferritin showed area under the curve (AUC) of 0.79 (p < 0.001) for the cut-off of 1873.0 ng/mL, sensitivity of 68.4% and specificity of 79.3% in predicting in-hospital mortality. Age ≥60 years had an odds ratio (OR) of 10.5 (95% CI = 1.8–59.5; p = 0.008) and ferritin ≥1873.0 ng/mL had an OR of 6.0 (95% CI = 1.4–26.2; p = 0.016), both independently associated with mortality based on logistic regression analysis.

Conclusion:

The magnitude of inflammation present at admission of COVID-19 patients, represented by high ferritin levels, is independently predictive of in-hospital mortality.

Keywords:
SARS-CoV-2; Ferritin; Mortality; Cytokine storm; Hemophagocytic lymphohistiocytosis

Introduction

It is known that some COVID-19 patients have poor outcomes and the factors responsible for determining these unfavorable evolution are still unsuccessfully understood. However, age and some comorbidities such as diabetes and hypertension were the first conditions thought to be risk factors for severe COVID-19.¹1 Argenziano MG, Bruce SL, Slater CL, et al. Characterization and clinical course of 1000 patients with coronavirus disease 2019 in New York: retrospective case series. BMJ. 2020;369:m1996.

Since SARS CoV-2 is a novel virus causing infection in humans, there is substantial uncertainty about how early clinical or laboratory findings could be related to infectivity and disease severity, besides how these parameters could contribute to increase mortality. In this context, studies have shown that the exacerbated inflammatory response (cytokine storm) can directly impair organ function in COVID-19 patients with moderate to severe disease, leading to decompensation, organ dysfunction and death.²2 Garcia LF. Immune response, inflammation, and the clinical spectrum of COVID-19. Front Immunol. 2020;11:1441.

In this report, we aimed to study the relationship between serum ferritin levels, measured at the moment of hospitalization, and general mortality among COVID-19 patients admitted to a high complexity university hospital. In addition, we also investigated if there is a ferritin cut-off value that could be predictive of death as the final outcome, which could be very useful in clinical practice for following up moderate to severe COVID-19 cases.

Material and methods

Study design

We retrospectively studied patients diagnosed with SARS-CoV-2 infection during the period of May through July 2020. This study focused on the analysis of common determinants and laboratory results obtained in the first days following hospital admission which could be associated with clinical outcomes (survival or death). In addition, cytomegalovirus (CMV) viral load was investigated since immunocompromised patients receives care at our hospital, where CMV infection could be an important cause of morbidity and mortality. This study was approved by the Ethics Committee of the Universidade Federal Fluminense (CAAE: 30623520.5.0000.5243).

Patients and data collection

Patients included in this study were admitted to the Hospital Universitario Antônio Pedro (HUAP – Niterói, Rio de Janeiro, Brazil) during the initial phase of COVID-19 pandemic in Brazil. HUAP is a reference hospital for the Metropolitan Region II of Rio de Janeiro State, which encompasses seven municipalities (about two million inhabitants). So, HUAP is the reference center for high complexity cases in this region, which includes cancer, autoimmune disease, heart surgeries, and transplants; being also the current reference treatment center for moderate to severe COVID-19 cases (e.g. persistent cough, fever and respiratory discomfort or drop in oxygen saturation). Included patients had detected RT-PCR for SARS-CoV-2 within the first week from the onset of symptoms. Patient data (e.g. sex, ethnicity, age, and comorbidities such as cancer, diabetes, immunosuppressive disorders, cardiovascular and chronic kidney diseases) were retrieved from medical charts.

Diagnosis of SARS-CoV-2 infection

During the COVID-19 pandemic, the Multiuser Laboratory for Research Support in Nephrology and Medical Science (LAMAP) located at HUAP has been equipped to perform RNA extraction and RT-PCR to diagnose SARS-CoV-2 infection, operating in accordance with the Brazilian Ministry of Health regulations. Briefly, viral RNA was isolated from nasopharyngeal swabs or tracheal aspirates from subjects with suspected COVID-19 using the QIAamp Viral RNA kit (Catalog no. 52906, QIAGEN, Hilden, Germany) according to the manufacturer's instructions. Subsequently, using the 2019-nCOV RUO Kit (Catalog no. 10006770, Integrated DNA Technologies, Inc – IDT, Iowa, USA) and GoTaq^® Probe 1-Step RT-qPCR (Catalog no. A6121, Promega Corporation, Wisconsin, USA) the assay was performed in three separate reactions per specimen for each target (N1, N2, and the internal control RNAaseP). Finally, amplification was performed using the 7500 System (Applied Biosystems, ThermoFisher Scientific, California, USA).

Laboratory tests

Biochemical and hematological parameters were assessed by automated methods using Siemens Dimension RxL MaxR (Siemens, Newark, Delaware, USA), Coulter LH 750R (Beckman Coulter, California, USA) and Sysmex CA-1500 SystemR (Sysmex America Inc., Illinois, USA) equipments. International normalized ratio (INR) was calculated. Leukopenia was defined as a value lower than 4000 leukocytes/mm³ and lymphopenia as a value lower than 1000 lymphocytes/mm³. All the routine tests were performed at the Clinical Pathology Service (HUAP/UFF).

Statistical analysis

Data are expressed as mean ± standard deviation (SD) or n (%). We divided the cases into two groups at the end of hospitalization time: patients who remained alive and patients who had died. For continuous variables, differences between two groups or more were assessed by t test or Mann–Whitney test and ANOVA or Kruskal–Wallis test with the correspondent post-tests, according to the variable distribution. Two-sided chi-square test was used to compare differences between proportions of categorical variables. The ability of a test to predict the primary clinical outcome or status (hospital discharge vs. death) was evaluated by the area under curve (AUC) after performing a receiver operating characteristic curve (ROC). Subsequently, using cut-offs for a variable, we performed the calculation of positive and negative predictive values. For the stepwise logistic regression, all variables presenting p-value ≤0.1 in uni-variate analysis were included in the initial binary model considering outcome (survival or death) as the dependent variable to estimate odds ratios (OR). Data were analyzed using statistical package (SPSS) and p-values were considered significant when <0.05.

Results

During the months of May through July 2020, we received respiratory tract samples of hospitalized patients to assess COVID-19 suspected cases. A total of 97 SARS-CoV-2 positive patients were diagnosed. The overall mean age (±SD) was 59.9 ± 16.3 years, 57/97 (58.8%) were male; 42.3% self-declared to be white, 9.3% black, 23.7% brown, 1.0% Asian, and that was no information for 23.7%. According to clinical severity, patients were admitted at the emergence room, infectious disease unit or intensive care unit. General symptoms presented at the time of hospital admission were mainly fever, cough, sore throat, sneezing, loss of taste, and eventually diarrhea or abdominal pain. In general, prostration and prominent dyspnea with O₂ saturation <95% associated to a ground glass pattern on thoracic tomography (>50%) were also frequently observed (cases were moderate to severe), constituting a typical presentation of hospitalized cases in our center. Overall, 44 (45.4%) patients died due to COVID-19. Biochemistry tests were performed within the first 24–48 h of hospitalization. We carefully checked the exact day of respiratory samples collection for SARS-CoV-2 detection and the day of symptoms onset. In our institution we have a CMV screening routine for laboratory monitoring in immunosuppressive patients and these results were also included, but with no statistical significance.

As shown in Table 1, the first part of the evaluation was a univariate analysis comparing the two groups (survival vs. death). Overall, there were statistical differences in age (p < 0.001), serum levels of ferritin (p < 0.05), C-reactive protein (p < 0.001), albumin (p < 0.05), and creatinine (p < 0.05). In addition, admission to intensive care unit (ICU) was also significantly associated (p < 0.0001). Importantly, serum ferritin levels at admission were not statically different between patients with and without immunosuppressive conditions (2661 ± 3188 ng/mL vs. 3028 ± 3644 ng/mL, respectively; p = 0.9).

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Table 1
Demographic and laboratory characteristics of 97 hospitalized SARS-CoV-2 positive patients according to survival status at the end of the study.

We also performed an analysis of demographic, clinical and laboratory parameters of COVID-19 hospitalized patients according to quartiles of serum ferritin obtained at admission. Patients with the highest ferritin levels (Q4 – ferritin of 3345–14,660 ng/mL) also presented significant higher levels of C-reactive protein (p < 0.005) and serum creatinine (p = 0.04). These patients also had significantly lower levels of hemoglobin (p = 0.03) and serum albumin (p = 0.04). Finally, we observed an increased frequency of death by COVID-19 in the highest ferritin quartile (p = 0.003), where 75% of patients in the highest quartile evolved to death. These data are presented in Table 2. Of note, we performed the analysis of other clinical parameters such as higher frequency of comorbidities according to quartiles of ferritin, but no significant differences were observed (data not shown).

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Table 2
Demographic and laboratory parameters of COVID-19 hospitalized patients according to ferritin quartiles.

Next, to further test the relationship between each evaluated variable and mortality, we performed a series of ROC curves analyses as seen in Table 1. For non-significant variables (as LDH, neutrophil and lymphocytes count, for example, the ROC curves had low AUC values and a p-value less than 0.05). For the variables with a significant p-value, (as age, ferritin, C-reactive protein, serum albumin and creatinine), we identified that only age and ferritin presented a value of AUC greater than 0.7 (0.72 and 0.79; respectively) using cut-offs of 60.0 years for age, and 1873.0 ng/mL for ferritin, respectively. Using this cut-off for ferritin, we observed sensitivity of 68.4% and specificity of 79.3%. Fig. 1 shows the display of ROC curve for ferritin.

Fig. 1
ROC curve for ferritin, with the grouping outcome of being alive or dead at the end of the study.

Lastly, we performed a logistic regression model for the analysis of age and serum ferritin as independent predictors of mortality. In this regard, based on a p < 0.1 in univariate analysis seen in Table 1, the following variables were included in a step-wise logistic regression model: age, ferritin, C-reactive protein, serum albumin, and creatinine. In the final model, only age ≥60.0 years-old (OR: 10.5; 95% CI = 1.8–59.5; p = 0.008) and ferritin ≥1873.0 ng/mL (OR: 6.0; 95% CI: 1.4–26.2; p = 0.016) remained independently associated with mortality. Table 3 shows the final logistic regression model.

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Table 3
Analysis of independent predictors of mortality in COVID-19 hospitalized patients using a logistic regression model.

Discussion

In December 2019, a new coronavirus was identified as responsible for cases of severe pneumonia, which was later called SARS-CoV-2.³3 Cruickshank M, Shaban RZ. COVID-19: lessons to be learnt from a once-in-a-century global pandemic. J Clin Nurs. 2020. The virus spread quickly worldwide and subsequently, the World Health Organization (WHO) declared its associated disease, COVID-19, as an international public health emergency.⁴4 Li X, Wang W, Zhao X, et al. Transmission dynamics and evolutionary history of 2019-nCoV. J Med Virol. 2020;92:501-11. Genome sequencing of this virus was carried out⁵5 Lu H, Stratton CW, Tang YW. Outbreak of pneumonia of unknown etiology in Wuhan, China: the mystery and the miracle. J Med Virol. 2020;92:401-2. and led to the development of specific diagnostic tests based on reverse transcription real time-PCR (RT-qPCR).⁶6 Henter JI, Horne A, Arico M, et al. HLH-2004: diagnostic and therapeutic guidelines for hemophagocytic lymphohistiocytosis. Pediatr Blood Cancer. 2007;48:124-31.

The acute phase reaction of an inflammatory process consists of a series of physiological and metabolic changes that begin immediately after tissue injury.⁷7 de Lucena TMC, da Silva Santos AF, de Lima BR, de Albuquerque Borborema ME, de Azevedo Silva J. Mechanism of inflammatory response in associated comorbidities in COVID-19. Diabetes Metab Syndr. 2020;14:597-600. Among the numerous systemic manifestations of this acute phase reaction is the variation in the concentrations of various plasma proteins, which are called “acute phase proteins”. Among these, the best known in clinical practice are C-reactive protein, amyloid substance serum A, haptoglobin, fibrinogen and ferritin.⁸8 Lagadinou M, Salomou EE, Zareifopoulos N, Marangos M, Gogos C, Velissaris D. Prognosis of COVID-19: changes in laboratory parameters. Infez Med. 2020;28(Suppl. 1):89-95. Serum ferritin has been long studied as a marker of iron metabolism,⁹9 Kell DB, Pretorius E. Serum ferritin is an important inflammatory disease marker, as it is mainly a leakage product from damaged cells. Metallomics. 2014;6:748-73. however, its application as biomarker of inflammation has far presented high importance in the context of COVID-19 progression, as demonstrated by previous studies in the field.¹⁰10 Henry BM, de Oliveira MHS, Benoit S, Plebani M, Lippi G. Hematologic, biochemical and immune biomarker abnormalities associated with severe illness and mortality in coronavirus disease 2019 (COVID-19): a meta-analysis. Clin Chem Lab Med. 2020;58:1021-8. Ferritin is an acute phase reactant, and as such, is generally elevated in inflammatory responses of any type. An initial assessment to identify the laboratory findings most commonly associated with the cytokine storm syndromes include a complete blood count, serum levels of ferritin, liver function tests, and others. These tests are readily available in the majority of health care facilities.

We studied, at the first days of hospital admission, a series of SARS-CoV-2 infected patients and we observed a strong correlation between serum ferritin and overall mortality, independently of age. A worse prognosis frequently is associated with a more rapid evolution to intensive and respiratory care or even dialysis. This is a concise laboratory-based report, which sought to answer whether we are able to identify any relevant role for risk prognosis using complementary tests routinely requested in positive SARS-CoV-2 hospitalized patients. The magnitude of the inflammation the patient already has at admission when the RT-PCR for SARS-CoV-2 is performed, seems to have a prognostic value.

There is increasing evidence that circulating ferritin levels may not only reflect an acute phase response but may play a critical role in inflammation.¹¹11 Torti FM, Torti SV. Regulation of ferritin genes and protein. Blood. 2002;99:3505-16. For most clinicians dealing with inflammatory diseases, serum ferritin levels are a rather non-specific marker of the acute phase response, which is often ignored or not measured when the patient is acutely ill. In some diseases, ferritin levels may be extremely high and, while not specific, these very high levels may be helpful in identifying patients at risk.¹²12 Rosario C, Zandman-Goddard G, Meyron-Holtz EG, D’Cruz DP, Shoenfeld Y. The hyperferritinemic syndrome: macrophage activation syndrome, Still's disease, septic shock and catastrophic antiphospholipid syndrome. BMC Med. 2013;11:185. In some previous studies, ferritin levels were more elevated in older and/or hypertensive participants, which was also associated with increased mortality.¹³13 Taneri PE, Gomez-Ochoa SA, Llanaj E, et al. Anemia and iron metabolism in COVID-19: a systematic review and meta-analysis. Eur J Epidemiol. 2020;35:763-73.

We emphasize that the profile of COVID-19 patients in our hospital is different from the general population, as they have advanced age, cardiovascular disease and diabetes, all correlated with higher mortality. We are a reference center for high complexity cases in our region. We highlight that 48.6% of our population had onco-hematological diseases and 22.0% had chronic kidney disease. A very relevant point in this study is the searching for a complementary routine exam that could be used as an independent predictor of mortality at the time of hospital admission.

In our study, CMV viral load at admission was not significantly correlated with final outcomes. CMV reactivation and risk for CMV disease possibly related with a subjacent immunosuppressive status may occur as in systemic lupus erythematous or in organ transplant¹⁴14 Lino K, Trizzotti N, Carvalho FR, et al. Pp65 antigenemia and cytomegalovirus diagnosis in patients with lupus nephritis: report of a series. J Bras Nefrol. 2018;40:44-52.^,¹⁵15 Carvalho FR, Cosendey RI, Souza CF, et al. Clinical correlates of pp65 antigenemia monitoring in the first months of post kidney transplant in patients undergoing universal prophylaxis or preemptive therapy. Braz J Infect Dis. 2017;21:51-6.; however, characteristics of latency and reactivation of the herpes family should be better monitored in the critically ill COVID-19 patients. For example, many of the reported cases and series of CMV-associated to cytokine storm syndromes involve viral reactivation during immune suppressed states.¹⁶16 Brisse E, Imbrechts M, Mitera T, et al. Lytic viral replication and immunopathology in a cytomegalovirus-induced mouse model of secondary hemophagocytic lymphohistiocytosis. Virol J. 2017;14:240. The rate of CMV seroprevalence increases with age. CMV has been shown to affect peripheral T cell phenotypes, increase inflammatory mediated cytokines such as IL-6 and play a role in immune dysregulation. The role of CMV in those with severe COVID-19 disease merits exploration.¹⁷17 Kadambari S, Klenerman P, Pollard AJ. Why the elderly appear to be more severely affected by COVID-19: the potential role of immunosenescence and CMV. Rev Med Virol. 2020;30:e2144.

A study focusing on early hyperinflammation in COVID-19 patients evaluated the high levels of serum ferritin in the first seven days of hospitalization as a predictor for the cytokine storm syndrome,¹⁸18 Caricchio R, Gallucci M, Dass C, et al. Preliminary predictive criteria for COVID-19 cytokine storm. Ann Rheum Dis. 2020. and a meta-analysis including 21 studies (3377 patients and 33 laboratory parameters) also demonstrated serum ferritin as a biomarker for potential progression to critical illness.¹⁰10 Henry BM, de Oliveira MHS, Benoit S, Plebani M, Lippi G. Hematologic, biochemical and immune biomarker abnormalities associated with severe illness and mortality in coronavirus disease 2019 (COVID-19): a meta-analysis. Clin Chem Lab Med. 2020;58:1021-8. Nevertheless, recent studies have also demonstrated that anti-inflammatory biomarkers could also be elevated during the acute phase of COVID-19.¹⁹19 Henry BM, Benoit SW, Vikse J, et al. The anti-inflammatory cytokine response characterized by elevated interleukin-10 is a stronger predictor of severe disease and poor outcomes than the pro-inflammatory cytokine response in coronavirus disease 2019 (COVID-19). Clin Chem Lab Med. 2020;59(3):599-607, http://dx.doi.org/10.1515/cclm-2020-1284. Print 2021 Feb 23.
http://dx.doi.org/10.1515/cclm-2020-1284... ^,²⁰20 Kox M, Waalders NJB, Kooistra EJ, Gerretsen J, Pickkers P. Cytokine levels in critically ill patients with COVID-19 and other conditions. JAMA. 2020;324:1565-7. This highlights the importance of future studies focusing on the balance between pro- and anti-inflammatory mediators and how this could impact on disease progression.

In conclusion, this study was designed to answer whether one could identify any relevant role for prognostic risk using routine complementary exams. The magnitude of the inflammation in the first days after hospitalization, represented by a hyperferritinemic syndrome, may help to identify patients at higher risk for early clinical decisions regarding the preventive measures directed at such patients.

Funding

This study was financed in part by the Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES, #001), Conselho Nacional de desenvolvimento Científico e Tecnológico (CNPq), Ministério da Educação (UFF) and The Brazilian Innovation Agency (FINEP) through Ministério da Ciência, Tecnologia e Inovações – REDE VÍRUS/Laboratórios de Campanha.

Acknowledgements

We would like to thank the Service of Clinical Pathology for laboratory tests and others undergraduate students that contribute to discussion of the manuscript, as Gilmar de Souza Lacerda.

References

¹
Argenziano MG, Bruce SL, Slater CL, et al. Characterization and clinical course of 1000 patients with coronavirus disease 2019 in New York: retrospective case series. BMJ. 2020;369:m1996.
²
Garcia LF. Immune response, inflammation, and the clinical spectrum of COVID-19. Front Immunol. 2020;11:1441.
³
Cruickshank M, Shaban RZ. COVID-19: lessons to be learnt from a once-in-a-century global pandemic. J Clin Nurs. 2020.
⁴
Li X, Wang W, Zhao X, et al. Transmission dynamics and evolutionary history of 2019-nCoV. J Med Virol. 2020;92:501-11.
⁵
Lu H, Stratton CW, Tang YW. Outbreak of pneumonia of unknown etiology in Wuhan, China: the mystery and the miracle. J Med Virol. 2020;92:401-2.
⁶
Henter JI, Horne A, Arico M, et al. HLH-2004: diagnostic and therapeutic guidelines for hemophagocytic lymphohistiocytosis. Pediatr Blood Cancer. 2007;48:124-31.
⁷
de Lucena TMC, da Silva Santos AF, de Lima BR, de Albuquerque Borborema ME, de Azevedo Silva J. Mechanism of inflammatory response in associated comorbidities in COVID-19. Diabetes Metab Syndr. 2020;14:597-600.
⁸
Lagadinou M, Salomou EE, Zareifopoulos N, Marangos M, Gogos C, Velissaris D. Prognosis of COVID-19: changes in laboratory parameters. Infez Med. 2020;28(Suppl. 1):89-95.
⁹
Kell DB, Pretorius E. Serum ferritin is an important inflammatory disease marker, as it is mainly a leakage product from damaged cells. Metallomics. 2014;6:748-73.
¹⁰
Henry BM, de Oliveira MHS, Benoit S, Plebani M, Lippi G. Hematologic, biochemical and immune biomarker abnormalities associated with severe illness and mortality in coronavirus disease 2019 (COVID-19): a meta-analysis. Clin Chem Lab Med. 2020;58:1021-8.
¹¹
Torti FM, Torti SV. Regulation of ferritin genes and protein. Blood. 2002;99:3505-16.
¹²
Rosario C, Zandman-Goddard G, Meyron-Holtz EG, D’Cruz DP, Shoenfeld Y. The hyperferritinemic syndrome: macrophage activation syndrome, Still's disease, septic shock and catastrophic antiphospholipid syndrome. BMC Med. 2013;11:185.
¹³
Taneri PE, Gomez-Ochoa SA, Llanaj E, et al. Anemia and iron metabolism in COVID-19: a systematic review and meta-analysis. Eur J Epidemiol. 2020;35:763-73.
¹⁴
Lino K, Trizzotti N, Carvalho FR, et al. Pp65 antigenemia and cytomegalovirus diagnosis in patients with lupus nephritis: report of a series. J Bras Nefrol. 2018;40:44-52.
¹⁵
Carvalho FR, Cosendey RI, Souza CF, et al. Clinical correlates of pp65 antigenemia monitoring in the first months of post kidney transplant in patients undergoing universal prophylaxis or preemptive therapy. Braz J Infect Dis. 2017;21:51-6.
¹⁶
Brisse E, Imbrechts M, Mitera T, et al. Lytic viral replication and immunopathology in a cytomegalovirus-induced mouse model of secondary hemophagocytic lymphohistiocytosis. Virol J. 2017;14:240.
¹⁷
Kadambari S, Klenerman P, Pollard AJ. Why the elderly appear to be more severely affected by COVID-19: the potential role of immunosenescence and CMV. Rev Med Virol. 2020;30:e2144.
¹⁸
Caricchio R, Gallucci M, Dass C, et al. Preliminary predictive criteria for COVID-19 cytokine storm. Ann Rheum Dis. 2020.
¹⁹
Henry BM, Benoit SW, Vikse J, et al. The anti-inflammatory cytokine response characterized by elevated interleukin-10 is a stronger predictor of severe disease and poor outcomes than the pro-inflammatory cytokine response in coronavirus disease 2019 (COVID-19). Clin Chem Lab Med. 2020;59(3):599-607, http://dx.doi.org/10.1515/cclm-2020-1284 Print 2021 Feb 23.
» http://dx.doi.org/10.1515/cclm-2020-1284
²⁰
Kox M, Waalders NJB, Kooistra EJ, Gerretsen J, Pickkers P. Cytokine levels in critically ill patients with COVID-19 and other conditions. JAMA. 2020;324:1565-7.

Publication Dates

Publication in this collection
16 June 2021
Date of issue
2021

History

Received
16 Oct 2020
Accepted
10 Feb 2021

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial No Derivative License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium provided the original work is properly cited and the work is not changed in any way.

[1] Funding

This study was financed in part by the Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES, #001), Conselho Nacional de desenvolvimento Científico e Tecnológico (CNPq), Ministério da Educação (UFF) and The Brazilian Innovation Agency (FINEP) through Ministério da Ciência, Tecnologia e Inovações – REDE VÍRUS/Laboratórios de Campanha.

Parameters	Total	Hospital discharge	Death	p
Age (years), mean ± SD (n)	59.9 ± 16.3 (97)	54.3 ± 17.1 (53)	66.7 ± 12.4 (44)	<0.001
Sex, (M/F) % of male	(57/40) 58.8%	(28/25) 52.8%	(29/15) 65.9%	0.219
Time between symptoms - PCR, mean ± SD (n)	5.3 ± 3.5 (53)	5.1 ± 3.8 (26)	5.5 ± 3.4 (27)	0.740
Cancer-hematology, (Yes/No) % of Yes	(34/36) 48.6%	(14/21) 40.0%	(20/15) 57.1%	0.232
UTI admission, (Yes/No) % of Yes	(40/30) 57.1%	(12/23) 34.3%	(28/7) 80.0%	0.000
Diabetes, (Yes/No) % of Yes	(27/43) 38.6%	(13/22) 37.1%	(14/21) 40.0%	1.000
Immunosuppressed status, (Yes/No) % of Yes	(11/59) 15.7%	(5/30) 14.3%	(6/29) 17.1%	1.000
CVD, (Yes/No) % of Yes	(47/22) 68.1%	(22/12) 64.7%	(25/10) 71.4%	0.611
CKD, (Yes/No) % of Yes	(16/54) 22.9%	(5/30) 14.3%	(11/24) 31.4%	0.153
Nosocomial infection, (Yes/No) % of Yes	(10/87) 10.3%	(3/50) 5.7%	(7/37) 9.1%	0.178
Hemoglobin, mean ± SD (n)	10.2 ± 2.5 (93)	10.6 ± 2.2 (50)	9.9 ± 2.8 (43)	0.682
Leukopenia, (Yes/No) % of Yes	(16/76) 17.4%	(6/43) 12.2%	(10/33) 23.2%	0.181
Lymphopenia, (Yes/No) % of Yes	(49/42) 53.8%	(23/26) 46,9%	(26/16) 61.9%	0.206
Platelets ×10³, mean ± SD (n)	237.8 ± 132.1 (93)	241.4 ± 133.4 (50)	233.7 ± 132.0 (43)	0.781
Ferritin, mean ± SD (n)	2703.4 ± 3305.2 (48)	1717.7 ± 2789.8 (29)	4207.7 ± 3530.3 (19)	<0.05
C-reactive protein, mean ± SD (n)	15.3 ± 13.2 (85)	8.5 ± 7.9 (44)	22.6 ± 13.9 (41)	<0.001
Albumin, mean ± SD (n)	3.1 ± 0.6 (40)	3.29 ± 0.54 (21)	2.91 ± 0.60 (19)	<0.05
AST, mean ± SD (n)	48.8 ± 65.0 (59)	38.7 ± 30.5	59.9 ± 88.4	0.236
ALT, mean ± SD (n)	30.1 ± 31.4 (59)	33.3 ± 39.6 (31)	27.6 ± 19.1 (28)	0.485
Total bilirubin, mean ± SD (n)	1.0 ± 1.8 (44)	0.73 ± 1.09 (26)	1.28 ± 2.49 (18)	0.394
LDH, mean ± SD (n)	449.0 ± 862.3 (45)	508.0 ± 1155.1 (25)	375.2 ± 161.8 (20)	0.575
D dimer, mean ± SD (n)	2698.4 ± 2497.0 (70)	2428.6 ± 2808.6 (37)	3000.9 ± 2095.6 (33)	0.334
Creatinine, mean ± SD (n)	1.8 ± 1.9 (89)	1.44 ± 1.81 (46)	2.26 ± 1.91 (43)	<0.05
qPCR CMV, (pos/neg) % of positives	(6/57) 9.5%	(4/26) 13.3%	(2/31) 6.1%	0.412

Parameters	Q1 (108-463.8)	Q2 (463.9-1425)	Q3 (1426-3344)	Q4 (3345-14,660)	p-Value
Age, mean ± SD	51.42 ± 20.16	63.33 ± 14.12	60.00 ± 15.82	66.50 ± 6.346	0.09
Death, %	0	42%	42%	75%	0.003
Hemoglobin, mean ± SD	10.61 ± 2.178	10.86 ± 2.107	10.34 ± 2.909	8.092 ± 1.962	0.03 ^b
Leukopenia, %	25%	17%	17%	33%	0.7
Lymphopenia, %	33%	42%	58%	50%	0.6
Platelets, mean ± SD	252.6 ± 155.1	257.3 ± 112.1	262.0 ± 104.2	186.0 ± 151.6	0.1
C-reactive protein, mean ± SD	9.581 ± 9.920	9.854 ± 9.745	10.44 ± 6.447	23.78 ± 9.402	<0.005 ^a,b,c
Albumin, mean ± SD	3.57 ± 0.53	3.04 ± 0.78	3.4 ± 0.38	2.58 ± 0.41	0.04 ^a
AST, mean ± SD	26.71 ± 21.08	42.50 ± 21.69	31.50 ± 17.25	91.73 ± 135.5	0.08
ALT, mean ± SD	24.14 ± 25.23	33.08 ± 30.94	22.88 ± 13.13	37.82 ± 31.73	0.7
Total bilirubin, mean ± SD	0.37 ± 0.37	0.43 ± 0.29	1.39 ± 1.66	2.04 ± 3.98	0.2
LDH, mean ± SD	258.8 ± 103.4	337.2 ± 163.9	309.6 ± 112.8	1157 ± 2158	0.5
D-dimer, mean ± SD	1628 ± 1484	2072 ± 2065	2369 ± 1798	3713 ± 2629	0.1
Creatinine, mean ± SD	0.85 ± 0.65	1.5 ± 1.1	1.2 ± 1.5	3.3 ± 3.4	0.004 ^a

Parameters	Wald	B	SE	Odds ratio	95% CI		p-Value
Parameters	Wald	B	SE	Odds ratio	Lower	Upper	p-Value
Age ≥ 60 years	7.038	2.350	0.886	10.490	1.848	59.555	0.008
Ferritin ≥ 1873 ng/mL	5.756	1.798	0.750	6.040	1.390	26.253	0.016

Brasil

Brasil

Serum ferritin at admission in hospitalized COVID-19 patients as a predictor of mortality

ABSTRACT

Introduction:

Objective:

Methods:

Results:

Conclusion:

Introduction

Material and methods

Study design

Patients and data collection

Diagnosis of SARS-CoV-2 infection

Laboratory tests

Statistical analysis

Results

Discussion

Acknowledgements

References

Publication Dates

History