Characteristics and predictors of outcomes of critically Ill children with SARS-CoV-2 infection - the PICU experience

Kazi, Maha Ashraf; Roychowdhury, Satyabrata; Ghosh, Sanajit; Mahapatra, Manas Kumar; Bhakta, Subhajit; Konar, Mithun Chandra; Sarkar, Mihir

doi:10.1016/j.jped.2021.12.006

Abstract

Objective

To describe the clinical characteristics, laboratory parameters, treatment, and predictors of an unfavorable outcome of critically ill children with SARS-CoV-2 infection.

Method

This was a prospective observational study performed in a pediatric intensive care unit (PICU) of a tertiary care COVID referral hospital among critically ill children in the age group 1 month - 12 years admitted due to SARS-CoV-2 infection from June to December 2020. Demographic, clinical profile, pSOFA and PRISM III scores, laboratory parameters, treatment, and outcomes of the patients were recorded. Children who had a prolonged PICU stay (>14 days) or died were compared with those who were discharged from PICU within 14 days to assess predictors of unfavorable outcomes.

Results

PICU admission rate among hospitalized SARS-CoV-2 infected children was 22.1% (92/416). Infants comprised the majority of the ICU population. Invasive mechanical ventilation and inotropic support were required for 28.3% and 37% of patients, respectively. Remdesivir, IVIg, and steroids were administered to 15.2%, 26.1%, and 54.3% of the subjects, respectively. The mortality rate was 7.6 %. MIS-C patients were older, less comorbid, and required less ventilator support but more inotrope support than acute severe COVID-19 patients. Predictors of unfavorable outcomes were age < 1 year, fever duration > 5 days, respiratory distress, shock, comorbidity, elevated CRP (> 50 mg/L), procalcitonin (> 6 ng/L), D-dimer (> 6 µg/L) and arterial lactate (> 2 mmol/L).

Conclusion

Critically ill children with unfavorable outcomes were predominantly infants, comorbid, prolonged fever, respiratory distress, shock and elevated inflammatory markers, D-dimer and lactate. These factors may be useful for watchful monitoring and early intervention.

Keywords
Critically ill children; COVID-19; PICU; Predictors of unfavorable outcome

Introduction

Coronavirus has taken the world by storm since its inception in Wuhan in December 2019.¹1 World Health Organization (WHO). Novel coronavirus - China [Internet]; 2020. [cited 6 January 2022]. Available from:https://www.who.int/emergencies/disease-outbreak-news/item/2020-DON233
https://www.who.int/emergencies/disease-... As evident from surveillance data from many countries, children have been less affected by the pandemic than adults accounting for 1-8% of the laboratory-confirmed cases.²2 Wu Z., McGoogan J.M. Characteristics of and important lessons from the coronavirus disease 2019 (COVID-19) outbreak in China: summary of a report of 72 314 cases from the Chinese Center for Disease Control and Prevention. JAMA. 2020;323:1239-42.

3 Statista. Age distribution of coronavirus (COVID-19) cases in South Korea as of July 24, 2020. [cited 29 July 2020]. Available from: https://www.statista.com/statistics/1102730/south-korea-coronavirus-cases-by-age/
https://www.statista.com/statistics/1102...

4 Posfay-Barbe K.M., Wagner N., Gauthey M., Moussaoui D., Loevy N., et al. COVID-19 in children and the dynamics of infection in families. Pediatrics. 2020;146:e20201576.

5 Docherty A.B., Harrison E.M., Green C.A., Hardwick H.E., Pius R., Norman L., et al. Features of 20 133 UK patients in hospital with covid-19 using the ISARIC WHO clinical characterisation protocol: prospective observational cohort study. BMJ. 2020;369:m1985.-⁶6 Stokes E.K., Zambrano L.D., Anderson K.N., Marder E.P., Raz K.M., El Burai Felix S., et al. Coronavirus disease 2019 case surveillance - United States, January 22-May 30, 2020. MMWR Morb Mortal Wkly Rep. 2020;69:759-65. As per the COVID-NET, the cumulative COVID-19 hospitalization rates for children less than 18 years are much lower than adults (8/100,000 population vs. 164.5/100,000 population), but ICU requirements among hospitalized children (33.2%) are similar to that of adults (32%).⁷7 Kim L., Whitaker M., O'Halloran A., Kambhampati A., Chai S.J., Reingold A., et al. Hospitalization rates and characteristics of children aged <18 years hospitalized with laboratory-confirmed COVID-19 - COVID-NET, 14 states, March 1-July 25, 2020. MMWR Morb Mortal Wkly Rep. 2020;69:1081-8.

Several studies have come up in the west demonstrating characteristics of critically ill children with COVID infection requiring ICU care.⁸8 Shekerdemian L.S., Mahmood N.R., Wolfe K.K., Riggs B.J., Ross C.E., McKiernan C.A., et al. Characteristics and outcomes of children with coronavirus disease 2019 (COVID-19) infection admitted to US and Canadian pediatric intensive care units. JAMA Pediatr. 2020;174:868-73.,⁹9 Swann O.V., Holden K.A., Turtle L., Pollock L., Fairfield C.J., Drake T.M., et al. Clinical characteristics of children and young people admitted to hospital with covid-19 in United Kingdom: prospective multicentre observational cohort study. BMJ. 2020;370:m3249. More cases of pediatric ARDS and septic shock syndromes among children with COVID infection have been reported over time.¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2. Currently, India stands amidst the second wave of the coronavirus pandemic, with 403,405 new cases reported on May 08, 2021.¹¹11 Johns Hopkins University. Center for systems science and engineering (CSSE). Novel coronavirus (COVID-19) cases, provided by JHU CSSE [Internet]. May 08, 2021. [cited 6 January 2022]. Available from: https://systems.jhu.edu/research/public-health/ncov/
https://systems.jhu.edu/research/public-... Also, with the detection of mutated strains (N440K and E484K) in some states of India, they have been found to be more transmissible than their predecessor strain¹²12 Mordani S. Govt confirms two new strains of Covid-19 in India. Here is all you need to know [Internet]. India Today 23 February 2021. [cited 1 April 2021]. Available from:https://www.indiatoday.in/coronavirus-outbreak/story/govt-confirms-two-new-strains-of-covid-19-in-india-here-is-all-you-need-to-know-1772313-2021-02-23
https://www.indiatoday.in/coronavirus-ou... ; there are concerns regarding increased disease severity and ICU requirements in children.

Sufficient data regarding characteristics of critically ill children with COVID infection and bad prognostic markers in resource-restricted settings are lacking. Through this study, the authors hope to provide an insight into the clinical characteristics, laboratory parameters, treatment, and outcomes and put forward specific predictors of an unfavorable outcome among the pediatric population infected by SARS-CoV-2 virus.

Materials and methods

This prospective observational study was conducted from June to December 2020 at a tertiary care teaching hospital in Eastern India dedicated to COVID care. Data collection was done after obtaining approval from the Institutional Ethics Committee (Ref no. - MC/KOL/IEC/NON-SPON/781/06/20). Informed consent/ assent was obtained from the legal guardian/ child enrolled in the study in their own language.

Children between 1 month - 12 years with evidence of SARS-CoV-2 infection in their nasopharyngeal swab RT-PCR requiring critical care support were included in the study. Those who needed PICU care of fewer than 24 hours for stabilization or refused to furnish assent/consent were excluded.

Demographic characteristics like age, sex, weight and contact history were collected. Presenting signs and symptoms and the presence of comorbidities with details of comorbid conditions were taken into account. Multisystem inflammatory syndrome in children associated with COVID-19 (MIS-C) was defined as per the WHO preliminary definition criteria.¹³13 World Health Organization (WHO). Multisystem inflammatory syndrome in children and adolescents with COVID-19. Scientific Brief, 15 May 2020. [cited 6 January 2022]. Available from:https://www.who.int/publications/i/item/multisystem-inflammatory-syndrome-in-children-and-adolescents-with-covid-19
https://www.who.int/publications/i/item/... PRISM III scores¹⁴14 Wang J.N., Wu J.M., Chen Y.J. Validity of the updated pediatric risk of mortality score (PRISM III) in predicting the probability of mortality in a pediatric intensive care unit. Acta Paediatr Taiwan. 2001;42:333-7. were calculated within 24 hours of admission, multiorgan dysfunction was assessed by Pediatric SOFA(p-SOFA)¹⁵15 Matics T.J., Sanchez-Pinto L.N. Adaptation and validation of a pediatric sequential organ failure assessment score and evaluation of the sepsis-3 definitions in critically Ill children. JAMA Pediatr. 2017;171:e172352. score.

Laboratory parameters following admission and hospital stay, including hematological parameters, coagulation tests, D-dimer, creatinine, urea, liver function markers and presence of coinfections, were assessed for every patient. Inflammatory markers such as C reactive protein (CRP), procalcitonin, ferritin, and Il-6 levels were measured. In patients with myocarditis, NT-ProBNP assay was performed. During the PICU stay, these investigations were performed on more than one occasion as per clinical indications, but the laboratory reports obtained within the first 48 hours of admission were taken for statistical analysis. All critically ill patients admitted in PICU were screened for bacterial coinfection by culture from a suitable sample and serology for tropical fevers like malaria, dengue, enteric fever, scrub typhus and leptospira.

For identifying predictors of unfavorable outcome the cut off values were taken as - elevated CRP (> 50 mg/L), high procalcitonin (> 6 µg/L), hyperferritinemia (> 1000 µg/L), high IL-6 (≥ 7 ng/L), raised pro-BNP ≥ 1000 ng/L), elevated D-dimer (> 6 µg/L).¹⁶16 Salto-Alejandre S., Roca-Oporto C., Martín-Gutiérrez G., Avilés M.D., Gómez-González C., Navarro-Amuedo M.D., et al. A quick prediction tool for unfavourable outcome in COVID-19 inpatients: development and internal validation. J Infect. 2021;82:e11-e15.,¹⁷17 Hariyanto T.I., Japar K.V., Kwenandar F., Damay V., Siregar J.I., Lugito N.P., et al. Inflammatory and hematologic markers as predictors of severe outcomes in COVID-19 infection: a systematic review and meta-analysis. Am J Emerg Med. 2021;41:110-9. The cut-off values for hematological were - anemia (Hb < 9 gm/dL), thrombocytopenia (platelet ≤ 150 × 10⁹/L), leucopenia (WBC < 4.5 × 10⁹/L), leucocytosis (WBC > 12 × 10⁹/L), Lymphopenia (< age-appropriate normative value) hypoalbuminemia (< 2.5 gm/dL) and deranged INR (> 1.5).

Chest X-Ray, lung ultrasound, and echocardiographic findings were recorded. Echocardiography was performed in patients with features of shock, unexplained tachycardia, and symptoms suggestive of MIS-C. Myocardial dysfunction was defined by the presence of global or segmental contractility alterations, ventricular dilatation, ejection fraction less than 55% measured by modified Simpson's method. A coronary artery Z score greater than +2 standard deviation was considered significant coronary artery dilatation. Bedside lung USG was performed by Philips HD7 (Philips Healthcare, Netherlands) with the high-frequency linear probe (L 7-12 mHz), and the lung USG score was calculated in 12 zones for patients¹⁸18 Volpicelli G., Elbarbary M., Blaivas M., Lichtenstein D.A., Mathis G., Kirkpatrick A.W., et al. International evidence-based recommendations for point-of-care lung ultrasound. Intensive Care Med. 2012;38:577-91.,¹⁹19 Ji L., Cao C., Gao Y., Zhang W., Xie Y., Duan Y., et al. Prognostic value of bedside lung ultrasound score in patients with COVID-19. Crit Care. 2020;24:700. with pulmonary involvement within 24 hours of admission. Presence > 3 B lines at a particular lung field is considered abnormal findings.

Treatment received by the patients such as type of highest respiratory support with the duration of ventilator days in those requiring invasive ventilation, inotropes/vasopressor requirement, highest Vasoactive inotrope score (VIS),²⁰20 McIntosh A.M., Tong S., Deakyne S.J., Davidson J.A., Scott H.F. Validation of the vasoactive-inotropic score in pediatric sepsis. Pediatr Crit Care Med. 2017;18:750-7. remdesivir, steroids, immunomodulators and additional supports like osmotherapy (3% NaCl) and renal replacement therapy were tabulated.

Septic shock, acute respiratory distress syndrome (ARDS) and acute kidney injury were defined and managed as per the Surviving Sepsis Campaign International Guidelines for the Management of Septic Shock in children,²¹21 Weiss S.L., Peters M.J., Alhazzani W., Agus M.S., Flori H.R., Inwald D.P., et al. Surviving sepsis campaign international guidelines for the management of septic shock and sepsis-associated organ dysfunction in children. Pediatr Crit Care Med. 2020;21:e52-e106. Pediatric Acute Lung Injury Consensus Conference (PALIC) definition²²22 Pediatric Acute Lung Injury Consensus Conference Group. Pediatric acute respiratory distress syndrome: consensus recommendations from the pediatric acute lung injury consensus conference. Pediatr Crit Care Med. 2015;16:428-39. and KDIGO guidelines²³23 Selewski D.T., Cornell T.T., Heung M., Troost J.P., Ehrmann B.J., Lombel R.M., et al. Validation of the KDIGO acute kidney injury criteria in a pediatric critical care population. Intensive Care Med. 2014;40:1481-8. respectively.

To measure the outcomes, children were segregated into two groups - Group A, favorable outcome group, which consisted of the patients discharged from PICU within 14 days, and Group B, unfavorable outcome group, which comprised children with prolonged PICU stay (> 14 days) and death. The authors also analyzed the length of PICU stay and hospital stay.

Statistical analysis

Data were analyzed using SPSS statistical package (IBM SPSS Statistics, Version 25.0. Armonk, NY: IBM Corp). Results were presented as frequency and percentages for categorical data and as mean, median, standard deviation, and interquartile ranges for continuous data. Relations between categorical variables were tested using Chi-square and Fisher's exact tests, and that between continuous variables was tested using Mann Whitney U or unpaired t-test. Risk factors for unfavorable outcomes were analyzed by univariate analysis followed by backward multivariate analysis of statistically significant factors (p-value < 0.05) identified by univariate analysis.

Results

During the study period, out of 416 confirmed Covid-19 infected hospitalized children, 92 (22.1%) required PICU support (Figure 1). The majority were infants 39 (42.4%) (Supplementary Table 1). Pneumonia (42.4%), shock (37%) and refractory convulsion (23.9%) were the leading reasons for PICU admission. Twenty (21.7%) patients satisfied the WHO preliminary case definition for MIS-C, out of whom 14 had shock or MODS and 6 presented with Kawasaki disease phenotype. Half of the patients (54.3%) had underlying comorbidities, most common being neurological disability (21.7%), hematological malignancies (10.9%), and congenital heart diseases (8.7%). Coinfections were present in 25% of the subjects. Mean PRISM III scores on the day of admission were (12.44 ± 8.45) whereas the highest mean pSOFA score during the stay was (12.74 ± 6.20).

Figure 1
Flowchart showing the admission pattern and outcome of pediatric COVID-19 patients at our centre.

The trends of laboratory parameters in the study sample are exhibited in Supplementary Table 2. Hemoglobin level was low (median Hb levels: 9.2 gm/dL), neutrophilic predominance and neutrophil/lymphocyte ratio was noted to be 5.2 (3.7- 10.3). Overall, thrombocytopenia was observed with a median value of 145 × 10⁹/L. Median CRP value was 48 mg/L (IQR - 6.7- 97.0). Other inflammatory markers like procalcitonin, IL-6, ferritin and NT pro-BNP showed higher than normal median values. Coagulation profile showed no significant variation from normal except D-dimer [4.7 µg/L (IQR 1.2 - 9.7)]. Forty-one (44.6%) of the children had abnormal infiltrates on chest radiography, predominantly of the diffuse type (22.8%). Lung USG exhibited the existence of abnormal findings in 54 subjects (58.7%), commonly B Lines (54.9%), pleural line abnormalities (48.3%), subpleural micro-consolidation (43.9%), and reduced lung sliding (34.06%).

Respiratory support in any form was needed for all critically ill patients. Among them, 26 (28.3%) required invasive mechanical ventilation (Supplementary Table 3). The mean duration of ventilator days was (7.8 ± 6.2) days. Proning was performed for 14/20 patients who met ARDS criteria. Inotrope/vasopressor support was needed in 37% of children, and the maximum VIS score was (54.7 ± 29.9). Remdesivir was administered to 14 (15.2%) children with severe disease and emergent or increasing need of oxygen within the first 10 days of illness. Intravenous immunoglobulin was employed in (26.1%) all patients of MIS-C and demyelinating lesions of the nervous system. Steroids were given to 50 (54.3 %) of the patients either with acute COVID-19 pneumonia/ARDS²³23 Selewski D.T., Cornell T.T., Heung M., Troost J.P., Ehrmann B.J., Lombel R.M., et al. Validation of the KDIGO acute kidney injury criteria in a pediatric critical care population. Intensive Care Med. 2014;40:1481-8. or MIS-C²⁰20 McIntosh A.M., Tong S., Deakyne S.J., Davidson J.A., Scott H.F. Validation of the vasoactive-inotropic score in pediatric sepsis. Pediatr Crit Care Med. 2017;18:750-7. or other indications like SVC syndrome and HLH (07).

Thirty-one (33.7%) of the patients had a prolonged PICU course (PICU stay >14 days or death). The overall mortality rate was 7.6% among PICU admitted patients. All deceased patients previously had debilitating chronic illnesses: one had a Gaucher disease, two had a relapse of acute lymphoblastic leukemia and severe immunodeficiency, two had multiple congenital anomalies with severe neurodisability, and two patients of systemic lupus erythematosus with multiorgan failure and immunodeficiency.

Univariate analysis revealed infants were more frequent in the unfavorable outcome group (67.7% vs. 39.3%, p-value 0.01) (Table 1). The proportion of patients with under-nutrition, presence of comorbidity, coinfections were significantly higher in children with unfavorable outcomes (p-value, 0.04, 0.003 and 0.039, respectively). Fever duration was significantly longer among children in Group B (10.74 ± 8.96 vs 6.49 ± 4.04, p = 0.025). Clinical presentation like respiratory distress, shock, and GCS < 7 at admission was associated with worsened prognosis.

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Table 1
Comparison of clinical characteristics, laboratory parameters and severity between children with favorable outcomes vs. children with unfavorable outcomes.

Hemoglobin levels, lymphocyte counts, platelet counts, albumin levels were lower, and total leucocyte counts, neutrophilic predominance, and inflammatory markers like CRP, procalcitonin, IL-6, pro-BNP, d-dimer, and blood lactate were significantly elevated in the unfavorable outcome group. The mean duration of PICU stay was significantly longer in children with unfavorable outcomes (15.2 ± 5.2 vs. 6.5 ± 4.3, p = 0.002).

On binary logistic regression analysis, it was revealed that as predictors for unfavorable outcome, adjusted odds ratio for infant age (OR- 2.58, p = 0.031), comorbidity (OR - 4.67, p= 0.002) was statistically significant (Table 2). Clinical features like prolonged fever > 5 days (OR - 3.54, p = 0.005), respiratory distress at admission (OR - 8.70, p = < 0.001), presence of shock (OR 3.39, p = 0.036) and GCS < 7 was significantly associated with unfavorable outcome. Need of invasive mechanical ventilatory support of day 1 was an independent worse outcome predictor. Among laboratory parameters elevated CRP > 50 mg/L (OR- 7.83, p ≤ 0.001), procalcitonin > 6 ng/L (OR-4.52, p = 0.004), D-dimer > 6 ng/L (OR- 3.88, p = 0.01) and arterial lactate > 2 mmol/L (OR- 5.65, p = 0.002) was observed to be significant unfavorable outcome predictors.

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Table 2
Binary logistic regression analysis for predictors of unfavourable outcomes among the study population.

Patients with MIS-C (20/72) were older than acute COVID patients (7.9 ± 3.6 vs 5.4 ± 4.8, p = 0.02) (Table 3). The prevalence of comorbidities was significantly higher in the latter. Shock, gastrointestinal and mucocutaneous symptoms predominated in the MIS-C group (p-value 0.003, 0.04, and 0.001 respectively). Respiratory involvement was more commonly noted in the acute COVID group. Laboratory parameters showed lower platelet counts higher CRP and ferritin levels in the MIS-C group. Coronary dilatation (6/20 vs 0/72) and myocardial dysfunction (p = 0.001) were more commonly observed in this group. Most patients in the MIS-C group recovered with non-rebreathing mask oxygen. Inotrope requirement and median VIS were significantly higher. IVIG and steroid were administered to all the MIS-C patients. Duration of PICU stay was shorter (7.08 ± 4.85 vs. 9.11 ± 5.14, p = 0.04), and no mortality was reported in MIS-C group.

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Table 3
Comparison of patients with acute covid infection and MIS-C.

Discussion

Characteristics of critically ill children with COVID-19 infection requiring PICU care have been described from western countries,⁸8 Shekerdemian L.S., Mahmood N.R., Wolfe K.K., Riggs B.J., Ross C.E., McKiernan C.A., et al. Characteristics and outcomes of children with coronavirus disease 2019 (COVID-19) infection admitted to US and Canadian pediatric intensive care units. JAMA Pediatr. 2020;174:868-73.

9 Swann O.V., Holden K.A., Turtle L., Pollock L., Fairfield C.J., Drake T.M., et al. Clinical characteristics of children and young people admitted to hospital with covid-19 in United Kingdom: prospective multicentre observational cohort study. BMJ. 2020;370:m3249.-¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁴24 Castagnoli R., Votto M., Licari A., Brambilla I., Bruno R., Perlini S., Rovida F, Baldanti F, Marseglia GL. et al. Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection in children and adolescents: a systematic review. JAMA Pediatr. 2020;174:882-9.

25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171.-²⁶26 Götzinger F., Santiago-García B., Noguera-Julián A., Lanaspa M., Lancella L., Calò Carducci F.I., et al. COVID-19 in children and adolescents in Europe: a multinational, multicentre cohort study. Lancet Child Adolesc Health. 2020;4:653-61. but literature is scarce from resource-restricted Asian counties. The authors observed that the PICU admission rates among COVID-19 hospitalized children was 22.1%. Infants were the most prevalent age group. Pneumonia, shock and refractory convulsion were the leading causes that called for PICU admission. Two-thirds of the patients were successfully discharged from PICU within 14 days. The mortality rate was 7.6%. Infant age group, presence of comorbidity, clinical presentations like either respiratory distress or shock or GCS < 7, laboratory parameters like elevated CRP, procalcitonin, D-dimer and arterial lactate were independently associated with unfavorable outcomes. Mean of maximum VIS score, PRISM III scores on admission, and highest pSOFA scores were double in the unfavorable outcome group.

Previous reports from all over the world mentioned a wide range of PICU admission rates (1.3-39%) among COVID-19 infected hospitalized children.⁹9 Swann O.V., Holden K.A., Turtle L., Pollock L., Fairfield C.J., Drake T.M., et al. Clinical characteristics of children and young people admitted to hospital with covid-19 in United Kingdom: prospective multicentre observational cohort study. BMJ. 2020;370:m3249.,¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171.,²⁶26 Götzinger F., Santiago-García B., Noguera-Julián A., Lanaspa M., Lancella L., Calò Carducci F.I., et al. COVID-19 in children and adolescents in Europe: a multinational, multicentre cohort study. Lancet Child Adolesc Health. 2020;4:653-61. A systematic review of the early period of the pandemic, Castagnoli et al.²⁴24 Castagnoli R., Votto M., Licari A., Brambilla I., Bruno R., Perlini S., Rovida F, Baldanti F, Marseglia GL. et al. Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection in children and adolescents: a systematic review. JAMA Pediatr. 2020;174:882-9. reported only one critically ill child among 1065 children (0.1%) from Asia with confirmed COVID-19. In a cohort of 77 hospitalized children from New York, 31 (39%) were cared for in the PICU; 14 (18.1%) had organ dysfunction and the majority (97%) survived to discharge.²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. Multicentre cohort study across 25 European countries, Götzinger et al. reported the PICU admission rate as 8%.²⁶26 Götzinger F., Santiago-García B., Noguera-Julián A., Lanaspa M., Lancella L., Calò Carducci F.I., et al. COVID-19 in children and adolescents in Europe: a multinational, multicentre cohort study. Lancet Child Adolesc Health. 2020;4:653-61. So it is evident that as the pandemic unfolded, a greater number of children required critical care support.

The present study found the clinical course and outcome of COVID-19 to be more severe in critically ill children than in studies from the USA.⁸8 Shekerdemian L.S., Mahmood N.R., Wolfe K.K., Riggs B.J., Ross C.E., McKiernan C.A., et al. Characteristics and outcomes of children with coronavirus disease 2019 (COVID-19) infection admitted to US and Canadian pediatric intensive care units. JAMA Pediatr. 2020;174:868-73.,¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. The mortality rate was recorded as 7.6% in the present study, whereas mortality ranged from 1.3 to 4% in reports from the USA. Swann et al. observed a mortality rate of 5% (6 out of 118) in PICU admitted patients in a multicenter study from the UK.⁹9 Swann O.V., Holden K.A., Turtle L., Pollock L., Fairfield C.J., Drake T.M., et al. Clinical characteristics of children and young people admitted to hospital with covid-19 in United Kingdom: prospective multicentre observational cohort study. BMJ. 2020;370:m3249. The higher mortality rate may be due to the fact that disease severity at presentation was higher in the study population as reflected in the p-SOFA score (12.74 ± 6.20) score compared to median p-SOFA score (3, IQR 2-7) among 14 PICU admitted children from New York.²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. Considering the early reports of very low mortality, an unfavorable outcome was defined if the patient required continuous PICU care for more than 14 days or was deceased in the study study cohort.

Data related to the association between comorbidity and more severe course and the unfavorable outcome is inconsistent among previously published literature. Shekerdemian et al. observed comorbidities were prevalent in 80% of the 48 children hospitalized with serious illness from Covid-19,⁸8 Shekerdemian L.S., Mahmood N.R., Wolfe K.K., Riggs B.J., Ross C.E., McKiernan C.A., et al. Characteristics and outcomes of children with coronavirus disease 2019 (COVID-19) infection admitted to US and Canadian pediatric intensive care units. JAMA Pediatr. 2020;174:868-73. whereas Fisler et al. concluded that the presence of underlying comorbidity was not associated with need for PICU admission (p = 0.227) or organ dysfunction (p = 0.87).²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. The authors found the presence of comorbidity was an independent predictor for unfavorable outcome. Question remains whether the severity of disease in these patients was solely due to comorbid condition (COVID as coincidental infection) or comorbid condition exacerbated by COVID-19 infection. Elezkurtaj et al. in autopsy series of adult COVID-19 patients, revealed that in the majority of decedents, causes of death were directly related to COVID-19, not an immediate result of pre-existing comorbidities.²⁷27 Elezkurtaj S., Greuel S., Ihlow J., Michaelis E.G., Bischoff P., Kunze C.A., et al. Causes of death and comorbidities in hospitalized patients with COVID-19. Sci Rep. 2021;11:4263.

The present study revealed infants were the most common age group (42.4%) requiring PICU care and was independently associated with unfavorable outcome. Initial reports from China reflected similar findings where severe and critical cases were reported in 10.6% of the children aged less than one year.²⁸28 Dong Y., Mo X., Hu Y., Qi X., Jiang F., Jiang Z., et al. Epidemiology of COVID-19 among children in China. Pediatrics. 2020;145:e20200702. However, multiple reports from the USA found that older children (> 12 yrs) were the most vulnerable group for PICU admission.¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. As the authors cater children up to 12 years of age at the study's centre it was not possible to draw a conclusion on adolescent age group.

Most common presenting symptoms across studies were pyrexia followed by symptoms of lower respiratory tract infection, reported in more than 70% of children.¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. Hypoxia, hemodynamic instability and radiological changes suggestive of pneumonia or ARDS were the most common indications for PICU admission.²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171.,²⁶26 Götzinger F., Santiago-García B., Noguera-Julián A., Lanaspa M., Lancella L., Calò Carducci F.I., et al. COVID-19 in children and adolescents in Europe: a multinational, multicentre cohort study. Lancet Child Adolesc Health. 2020;4:653-61. The almost identical observation was noticed in the present study's cohort; pneumonia, shock and refractory convulsion were the leading causes for PICU admission.

Among a large PICU population, 20 (28.6%) patients required invasive mechanical ventilation, 7 (10%) prone positioning, 1 (1.4%) extracorporeal membrane oxygenation (ECMO) and 14 (20%) supported with vasopressor.²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. Although being similar in a number of patients, inotrope/vasopressor support and mechanical ventilation were needed almost double in proportion in the present study. The mean duration of proning was 31.6 hours and the median ventilator stay was 6.7 days. The study centre doesn't have ECMO facility. Fourteen (15.2%) of the study's patients received remdesivir, particularly in those with severe disease and having respiratory involvement. Similar data were presented by Chao et al., remdesivir was administered in 18.3% of patients and the majority had ARDS.¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2. In view of the scant evidence available on the effectiveness of remdesivir therapy in children infected with SARS-CoV-2, further studies should be conducted to assess the efficacy.

Laboratory data from 8 severe pediatric cases showed normal or increased leukocyte count and high levels of C-reactive protein (CRP, procalcitonin, and LDH from China.²⁸28 Dong Y., Mo X., Hu Y., Qi X., Jiang F., Jiang Z., et al. Epidemiology of COVID-19 among children in China. Pediatrics. 2020;145:e20200702. Admission to an ICU and organ dysfunction was associated with higher WBC count, elevated CRP, procalcitonin, pro-BNP, and decreased platelet count.¹⁰10 Chao J.Y., Derespina K.R., Herold B.C., Goldman D.L., Aldrich M., Weingarten J., et al. Clinical characteristics and outcomes of hospitalized and critically Ill children and adolescents with coronavirus disease 2019 at a tertiary care medical center in New York City. J Pediatr. 2020;223:14-19.e2.,²⁵25 Fisler G., Izard S.M., Shah S., Lewis D., Kainth M.K., Hagmann S.H., et al. Characteristics and risk factors associated with critical illness in pediatric COVID-19. Ann Intensive Care. 2020;10:171. However, the authors found no association between total white blood cell count, absolute lymphocyte count, platelet count, and pro-BNP with unfavorable outcomes. The authors’ multivariate analysis revealed elevated CRP > 50 mg/L, procalcitonin > 6 ng/L, D-dimer > 6 ng/L and lactate > 2 mmol/L were predictors for unfavorable outcome.

Feldstein et al. compared patients with acute COVID-19 and MIS-C. MIS-C patients were younger and less likely to have a comorbidity.²⁹29 Feldstein L.R., Tenforde M.W., Friedman K.G., Newhams M., Rose E.B., Dapul H., et al. Characteristics and outcomes of US children and adolescents with multisystem inflammatory syndrome in children (MIS-C) compared with severe acute COVID-19. JAMA. 2021;325:1074-87. Higher CRP level and lower platelet count was observed among MIS-C group. The authors had similar observations except the older age group being more affected by MIS-C. This could be explained by the exclusion of adolescents more than 12yrs from the present study. Left ventricular dysfunction and coronary artery aneurysm were noted in 43.8% and 13.4% patients, respectively in the US study. As the authors included only PICU admitted patients, a higher LV dysfunction was found (80%) as well as coronary dilatation (30%) among MIS-C patients. Similar to the present study, García-Salido et al. found that patients in the MIS-C group were less likely to receive invasive ventilation (p = 0.005) but were more often treated with vasoactive drugs (p < 0.001).³⁰30 García-Salido A., de Carlos Vicente J.C., Belda Hofheinz S., Balcells Ramírez J., Slöcker Barrio M., Leóz Gordillo I., et al. Severe manifestations of SARS-CoV-2 in children and adolescents: from COVID-19 pneumonia to multisystem inflammatory syndrome: a multicentre study in pediatric intensive care units in Spain. Crit Care. 2020;24:666.

Limitations

The authors’ observational data was from a single centre and may not reflect the whole pediatric population as there may be variation in the spectrum of clinical characteristics, severity, and outcome. Lack of data of children above 12 years, one of the most affected ranges of age in children with COVID-19, is another limitation of the present study. Contribution of comorbid conditions vs. SARS-CoV-2 infection leading to critical illness in children with pre-existing comorbidity could not be ascertained definitely.

Conclusion

The authors have been able to highlight that infant age group, presence of comorbidity, either respiratory distress or shock or poor GCS, laboratory parameters like elevated CRP, procalcitonin and arterial lactate were independent predictors of unfavorable outcome in Covid-19 infected children, which necessitate the need for watchful monitoring and early intervention. Observation of the present research may help in the management of such critically ill pediatric populations in resource-restricted settings.

Supplementary materials

Supplementary material associated with this article can be found in the online version at doi:10.1016/j.jped.2021. 12.006.

Ethics approval

Approved by institutional Ethics committee and have therefore been performed in accordance with the ethical standards laid down in the 1964 Declaration of Helsinki and its later amendments.
Consent to participate

Informed consent and assent were obtained as applicable in understandable language.

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Publication Dates

Publication in this collection
24 Oct 2022
Date of issue
Sep-Oct 2022

History

Received
19 May 2021
Accepted
14 Dec 2021
Published
31 Jan 2022

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] Ethics approval

Approved by institutional Ethics committee and have therefore been performed in accordance with the ethical standards laid down in the 1964 Declaration of Helsinki and its later amendments.

[2] Consent to participate

Informed consent and assent were obtained as applicable in understandable language.

Parameter	Group A / favourable outcomen= 61	Group B / unfavourable outcomen= 31	ODDS ratio (95%CI)binary	p- value
Age < 1 year, n (%)	24 (39.3%)	21 (67.7%)	3.24 (1.2-9.04)	0.01
Male sex, n (%)	33 (54.1%)	18 (58.1%)	1.17 (0.45-3.11)	0.718
Underweight, n (%)	18 (29.5%)	18 (58%)	3.31 (1.22-8.99)	0.012
Presence of comorbidity, n (%)	28 (45.9%)	22 (70.9%)	2.8 (1.05-8.24)	0.028
Presence of Coinfection, n (%)	10 (16.4%)	11 (35.5%)	2.8 (0.91-8.59)	0.039
Clinical presentation
Fever duration in days (Mean, SD)	6.49, 4.03	10.74, 8.96		0.025
Duration of fever > 5 days, n (%)	21 (34.4)	19 (61.2)	3.02 (1.13-8.17)	0.016
Respiratory distress, n (%)	38 (62.3%)	29 (93.5%)	8.78 (2.16-27.21	0.001
Shock, n (%)	10 (16.4%)	24 (77.4%)	17.49 (5.32-30.08)	< 0.001
Convulsion, n (%)	13 (21.3%)	9 (29.0%)	1.15 (0.49-4.49)	0.412
Poor GCS (<7), n (%)	1 (1.6%)	10 (32.3%)	28.57 (6.55-59.77)	< 0.001
Oliguria, n (%)	4 (6.6%)	5 (16.1%)	2.74 (0.53-4.83)	0.144
Support parameters
Invasive Ventilation on Day 1, n (%)	8 (13.1)	18 (58)	9.17 (3.46- 25.78)	< 0.001
Laboratory parameters
Hb levels (gm/dL), Mean, SD	9.9, 2.2	7.7, 2.0		< 0.001
Hb < 9 gm/dL, n (%)	11 (185)	09 (29%)	1.86 (0.59-5.73)	0.287
Total leucocyte count (10⁹/L), Mean, SD	11.3, 8.8	15.5, 9.72		0.035
Leucocyte count >12.0 × 109 per L, n (%)	18 (29.5%)	23 (74.1)	6.87 (2.37-17.55)	0.001
Absolute Neutrophil count (10⁹/L),	8.6, 8.7	12.2, 9.5		0.02
Neutrophil count >7.5 × 109/L, n (%)	17 (27.8)	18 (58)	3.58 (1.32-9.8)	0.007
Absolute Lymphocyte count (10⁹/L), Mean, SD	2.3, 3.1	2.5, 3.4		0.199
Lymphopenia, n (%)	14 (22.9)	16 (51.6)	3.55 (1.29-9.96)	0.009
Neutrophil/ Lymphocyte ratio, Mean, SD	4.6, 3.2	6.3,5.2		0.01
Neutrophil/ Lymphocyte ratio > 3.5, n (%)	12	18	5.65 (1.97-16.36)	0.001
Platelet counts count (10⁹/L), Mean, SD	204, 112	145, 131		0.039
Platelet count < 150 × 109 per L, n (%)	7 (11.4)	11 (35.4)	4.42 (1.27-14.36)	0.01
CRP levels (mg/L), Mean, SD	39.7, 31.3	67.9, 48.8		0.002
CRP ≥ 50 mg/L, n (%)	5 (8.2)	12 (38.7)	7.07 (2.19-24.35)	0.001
Procalcitonin (µg/L), Mean, SD	4.6, 4.0	22.3, 18.8		0.001
Procalcitonin > 6µg/L, n (%)	8 (13.1)	18 (58)	9.17 (2.94- 19.5)	< 0.001
Ferritin (µg/L), Mean, SD	578.5, 423.6	1411.3, 1081.9		0.418
Ferritin ≥1000 ng/mL, n (%)	06 (9.84)	07 (22.5)	2.67 (0.68-10.64)	0.09
IL-6 (ng/L), Mean, SD	15.7, 11.4	35.0, 26.6		0.029
IL-6 > 7 ng/L, n (%)	12 (19.6)	13 (41.9)	2.95 (1.02-8.5)	0.028
NT pro-BNP (ng/L), Mean ± SD	3581.3,995.6	10131, 4447.7		0.184
NT pro-BNP > 1000 ng/L, n (%)	15 (24.5)	14 (45.1)	2.53 (0.91-6.95)	0.058
LDH (U/L), Mean ± SD	738.9, 872.5	1298.0, 2002.1		0.347
LDH ≥300 UI/L, n (%)	32 (52.4)	24 (77.7)	3.11 (1.08-9.75)	0.025
D-dimer(ng/L), Mean ± SD	4.9, 2.6	8.6, 7.2		0.02
D-dimer ≥ 6 ng/L, n (%)	5 (8.2)	13 (41.9)	8.09 (2.26-25.95)	0.001
Albumin (gm/L), Mean, SD	3.4, 0.7	2.8, 0.9		0.041
Albumin < 2.5 gm/L, n (%)	09 (14.7)	10 (32.2)	2.75 (0.86-8.80)	0.061
Arterial lactate, mmol/L Mean, SD	1.4, 1	3.1, 1.6		0.005
Arterial Lactate > 2 mmol/L, n (%)	4 (6.56)	12 (38.7)	5.9 (2.26-25.95)	0.001
SGOT (U/L), Mean, SD	134.3, 63.0	149.1, 81.8		0.903
SGPT (U/L) Mean, SD	69.6, 154.7	124.6, 251.4		0.199
Severity scores
Highest pSOFA score (Mean, SD)	9.9, 4.5	18.2, 5.4		< 0.001
PRISM III score on Day 1 (Mean, SD)	8.9, 6.2	19.5, 7.8		< 0.001
Highest VIS (Mean, SD)	34, 18.4	63.5, 30.4		0.007
Duration of PICU Stay (Mean, SD)	6.5,4.3	15.2, 5.2		0.002

Parameter	Adjusted odds ratio (OR)	95% Confidence interval (CI)	p-value
Age < 1 year	2.58	1.21-7.04	0.031
Presence of Comorbidity	4.67	1.25-8.64	0.002
Clinical parameters
Fever duration >5 days	3.54	1.23-7.26	0.005
Respiratory distress	8.70	2.16-20.10	< 0.001
Shock	3.39	1.02-8.08	0.036
Poor GCS (<7)	4.48	1.24-9.68	0.022
Support parameters
Need of Invasive Ventilation on Day 1	5.529	2.66- 9.78	0.003
Laboratory parameters
CRP levels > 50 mg/L	7.83	2.19-16.40	< 0.001
Procalcitonin > 6 ng/L	4.52	2.94- 8.58	0.004
D-dimer > 6 ng/L	3.88	1.26-7.64	0.010
Arterial lactate > 2 mmol/L	5.65	2.02-9.95	0.002
Severity scores
Highest pSOFA score > 8	4.58	1.24- 12.43	0.003
PRISM III score on Day 1 >11	4.59	1.03-11.64	0.003
Highest VIS (Mean, SD)> 20	2.43	0.7 - 5.68	0.034

Parameter	MIS-C(n= 20)	Acute Covid(n= 72)	p value
Age (Mean, SD)	7.9, 3.6	5.4, 4.8	0.02
Sex, Male n (%)	11 (55)	40 (56.3)	0.58
Nutrition status, underweight, n (%)	9 (45)	30 (41.6)	0.49
Presence of morbities, n (%)	4 (20)	46 (63.8)	0.001
Presence of fever, n (%)	20 (100%)	48 (66.7%)	0.001
Day of fever on presentation (Mean ± SD)	7.36 ± 8.86	7.94 ± 6.12	0.67
Respiratory involvement (Pneumonia/ARDS), n (%)	8 (40)	51 (70.8)	0.01
Shock, n (%)	14 (70)	20 (27.8)	0.001
Neurological, n (%)	4 (20)	25 (34.7)	0.28
Gastrointestinal (pain abdomen/loose stool/vomiting), n (%)	13 (65)	18 (25)	0.003
Mucocutaneous, n (%)	13 (65)	9 (12.5)	0.001
Echo cardiography, n (%)
Coronary dilatation	6 (30)	0 (0%)
Myocardial dysfunction (EF <55%)	16 (80)	5 (6.9)	0.001
Pericardial effusion	3 (15)	2 (2.8)	0.07
Hemoglobin level (gm/dL) Median (IQR)	9.1 (7-10.9)	9.25 (7.7-10.9)	0.077
Total Leucocyte Count (× 10⁹/L) Median (IQR)	13.26 (9.10-16.76)	12.37 (8.725-17.74)	0.640
Absolute Lymphocyte Count (× 10⁹/L) Median (IQR)	2.08 (1.24-3.03)	2.4 (1.27 -3.69)	0.468
Platelet count (× 10⁹/L) Median (IQR)	115 (372.50-231)	191 (235-500)	< 0.001
C Reactive Protein (mg/L) Median (IQR)	101.9 (68-134)	30 (5.9-86.7)	< 0.001
Ferritin (mcg/L) Median (IQR)	662 (278.7-1540)	380 (258-737)	0.025
Procalcitonin (mcg/L) Median (IQR)	12.47 (1.6-18.35)	1.9 (0.77-19)	0.07
Fibrinogen (mg/dL) Median (IQR)	301 (229-372.5)	109 (100-118)	0.072
Interleukin -6 (pg/ml) Median (IQR)	48.6 (21.6 - 66.8)	34.5 (9.5 - 50.4)	0.09
Respiratory support, n (%)
Non rebreathing mask	10 (50)	21 (29.1)	0.07
High flow nasal cannula	6 (30)	23 (31.94)	0.55
Invasive Mechanical Ventilation	4 (20)	22 (30.55)	0.41
Immunomodulators, n (%)
IVIG	20 (100)	04 (5.5)	0.001
Steroids	20 (100)	30 (41.66)	0.001
Biologics	1 (5)	3 (4.1)	0.246
Remdesivir, n (%)	2 (10)	12 (16.7)	0.72
Low Molecular Weight Heparin, n (%)	2 (10)	14 (19.4)	0.50
Inotropes, n (%)	16 (72.7)	18 (25)	0.001
VIS score, Median (IQR)	60 (40-80)	45 (25-65)	0.24
PICU stay in days (Mean ± SD)	7.08 ± 4.85	9.11 ± 5.14	0.04
Death	0	7 (100)

Brasil

Brasil

Characteristics and predictors of outcomes of critically Ill children with SARS-CoV-2 infection - the PICU experience

Abstract

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Introduction

Materials and methods

Statistical analysis

Results

Discussion

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