Multisystem Inflammatory Syndrome of Children: Subphenotypes, Risk Factors, Biomarkers, Cytokine Profiles, and Viral Sequencing

Roberta L DeBiasi; Ashraf S Harahsheh; Hemalatha Srinivasalu; Anita Krishnan; Matthew P Sharron; Kavita Parikh; Karen Smith; Michael Bell; Drew Michael; Meghan Delaney; Joseph Campos; Eric Vilain; Jonathan LoTempio; Jaclyn N Kline; Tova Ronis; Suvankar Majumdar; Eleanor Sadler; Susan R Conway; Charles I Berul; Sangeeta Sule; Rebeca Lahoz; Emily Ansusinha; Jay Pershad; Vanessa Bundy; Elizabeth Wells; James E Bost; David Wessel; Children's National Hospital MIS-C Taskforce

doi:10.1016/j.jpeds.2021.06.002

Multisystem Inflammatory Syndrome of Children: Subphenotypes, Risk Factors, Biomarkers, Cytokine Profiles, and Viral Sequencing

J Pediatr. 2021 Oct:237:125-135.e18. doi: 10.1016/j.jpeds.2021.06.002. Epub 2021 Jun 25.

Authors

Roberta L DeBiasi¹, Ashraf S Harahsheh², Hemalatha Srinivasalu³, Anita Krishnan², Matthew P Sharron⁴, Kavita Parikh⁵, Karen Smith⁵, Michael Bell⁴, Drew Michael⁶, Meghan Delaney⁷, Joseph Campos⁷, Eric Vilain⁸, Jonathan LoTempio⁸, Jaclyn N Kline⁹, Tova Ronis³, Suvankar Majumdar¹⁰, Eleanor Sadler¹¹, Susan R Conway⁴, Charles I Berul², Sangeeta Sule³, Rebeca Lahoz¹², Emily Ansusinha¹², Jay Pershad¹³, Vanessa Bundy¹⁴, Elizabeth Wells¹⁵, James E Bost¹⁶, David Wessel¹⁷; Children's National Hospital MIS-C Taskforce

Collaborators

Children's National Hospital MIS-C Taskforce:
Yasser Diab, Jessica Herstek, Sona Sehgal, Hemant Sharma, Andrea Hahn, Nada Harik, Rana Hamdy, Benjamin Hanisch, Barbara Jantausch, Adeline Koay, Bernhard Wiedermann, Alexandra Yonts, Xiaoyan Song, Jennifer Dien Bard

Affiliations

¹ Division of Pediatric Infectious Diseases, Children's National Hospital, Washington, DC; Division of Cardiology, Children's National Hospital, Washington, DC; Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Department of Microbiology, Immunology and Tropical Medicine, Washington, DC.
² Division of Cardiology, Children's National Hospital, Washington, DC; Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC.
³ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Rheumatology, Children's National Hospital, Washington, DC.
⁴ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Critical Care Medicine, Children's National Hospital, Washington, DC.
⁵ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Hospitalist Medicine, Children's National Hospital, Washington, DC.
⁶ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Laboratory Medicine and Pathology, Children's National Hospital, Washington, DC; Department of Pathology, The George Washington University School of Medicine and Health Sciences, Washington, DC; Department of Genomics and Precision Medicine, The George Washington University School of Medicine and Health Sciences, Washington, DC.
⁷ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Laboratory Medicine and Pathology, Children's National Hospital, Washington, DC.
⁸ Department of Genomics and Precision Medicine, The George Washington University School of Medicine and Health Sciences, Washington, DC; Center for Genetic Medicine Research, Children's Research Institute, Washington, DC.
⁹ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Emergency Medicine, Children's National Hospital, Washington, DC.
¹⁰ Division of Critical Care Medicine, Children's National Hospital, Washington, DC; Division of Hematology, Children's National Hospital, Washington, DC.
¹¹ Division of Pharmacy, The Mount Sinai Hospital, New York, New York.
¹² Division of Pediatric Infectious Diseases, Children's National Hospital, Washington, DC.
¹³ Division of Emergency Medicine, Children's National Hospital, Washington, DC.
¹⁴ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Immunology, Children's National Hospital, Washington, DC.
¹⁵ Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Neurology, Children's National Hospital, Washington, DC.
¹⁶ Division of Biostatistics, Children's National Hospital, Washington, DC.
¹⁷ Division of Cardiology, Children's National Hospital, Washington, DC; Department of Pediatrics, Immunology and Tropical Medicine, Washington, DC; Division of Critical Care Medicine, Children's National Hospital, Washington, DC.

PMID: 34181987
DOI: 10.1016/j.jpeds.2021.06.002

Abstract

Objective: To assess demographic, clinical, and biomarker features distinguishing patients with multisystem inflammatory syndrome in children (MIS-C); compare MIS-C sub-phenotypes; identify cytokine biosignatures; and characterize viral genome sequences.

Study design: We performed a prospective observational cohort study of 124 children hospitalized and treated under the institutional MIS-C Task Force protocol from March to September 2020 at Children's National, a quaternary freestanding children's hospital in Washington, DC. Of this cohort, 63 of the patients had the diagnosis of MIS-C (39 confirmed, 24 probable) and 61 were from the same cohort of admitted patients who subsequently had an alternative diagnosis (controls).

Results: Median age and sex were similar between MIS-C and controls. Black (46%) and Latino (35%) children were over-represented in the MIS-C cohort, with Black children at greatest risk (OR 4.62, 95% CI 1.151-14.10; P = .007). Cardiac complications were more frequent in critically ill patients with MIS-C (55% vs 28%; P = .04) including systolic myocardial dysfunction (39% vs 3%; P = .001) and valvular regurgitation (33% vs 7%; P = .01). Median cycle threshold was 31.8 (27.95-35.1 IQR) in MIS-C cases, significantly greater (indicating lower viral load) than in primary severe acute respiratory syndrome coronavirus 2 infection. Cytokines soluble interleukin 2 receptor, interleukin [IL]-10, and IL-6 were greater in patients with MIS-C compared with controls. Cytokine analysis revealed subphenotype differences between critically ill vs noncritically ill (IL-2, soluble interleukin 2 receptor, IL-10, IL-6); polymerase chain reaction positive vs negative (tumor necrosis factor-α, IL-10, IL-6); and presence vs absence of cardiac abnormalities (IL-17). Phylogenetic analysis of viral genome sequences revealed predominance of GH clade originating in Europe, with no differences comparing patients with MIS-C with patients with primary coronavirus disease 19. Treatment was well tolerated, and no children died.

Conclusions: This study establishes a well-characterized large cohort of MIS-C evaluated and treated following a standardized protocol and identifies key clinical, biomarker, cytokine, viral load, and sequencing features. Long-term follow-up will provide opportunity for future insights into MIS-C and its sequelae.

Keywords: COVID; SARS-CoV-2.

Publication types

Observational Study

MeSH terms

Adolescent
Biomarkers / blood
COVID-19 / blood
COVID-19 / diagnosis
COVID-19 / epidemiology
COVID-19 / immunology*
COVID-19 Nucleic Acid Testing
Cardiovascular Diseases / diagnosis
Cardiovascular Diseases / epidemiology
Cardiovascular Diseases / etiology*
Case-Control Studies
Child
Child, Preschool
Diagnosis, Differential
Female
Humans
Infant
Male
Pandemics
Phenotype
Phylogeny
Prospective Studies
Risk Factors
SARS-CoV-2 / immunology
Severity of Illness Index
Systemic Inflammatory Response Syndrome / blood
Systemic Inflammatory Response Syndrome / diagnosis
Systemic Inflammatory Response Syndrome / epidemiology
Systemic Inflammatory Response Syndrome / immunology*

Substances

Biomarkers

Supplementary concepts

pediatric multisystem inflammatory disease, COVID-19 related