MIS-C: A COVID-19-as sociated condition between hypoimmunity and hyperimmunity

Monica Gelzo; Alice Castaldo; Antonietta Giannattasio; Giulia Scalia; Maddalena Raia; Maria Valeria Esposito; Marco Maglione; Stefania Muzzica; Carolina D'Anna; Michela Grieco; Vincenzo Tipo; Antonio La Cava; Giuseppe Castaldo

doi:10.3389/fimmu.2022.985433

MIS-C: A COVID-19-as sociated condition between hypoimmunity and hyperimmunity

Front Immunol. 2022 Oct 3:13:985433. doi: 10.3389/fimmu.2022.985433. eCollection 2022.

Authors

Monica Gelzo^{1

2}, Alice Castaldo³, Antonietta Giannattasio⁴, Giulia Scalia¹, Maddalena Raia¹, Maria Valeria Esposito¹, Marco Maglione⁴, Stefania Muzzica⁴, Carolina D'Anna⁴, Michela Grieco⁴, Vincenzo Tipo⁴, Antonio La Cava^{2

5}, Giuseppe Castaldo^{1

2}

Affiliations

¹ CEINGE-Biotecnologie Avanzate, Scarl, Naples, Italy.
² Dipartimento di Medicina Molecolare e Biotecnologie Mediche, Università di Napoli Federico II, Naples, Italy.
³ Dipartimento di Scienze Mediche Traslazionali, Sezione di Pediatria, Università di Napoli Federico II, Naples, Italy.
⁴ Pediatric Emergency and Short Stay Unit, Santobono-Pausilipon Children's Hospital, Naples, Italy.
⁵ Department of Medicine, University of California, Los Angeles, Los Angeles, CA, United States.

Abstract

Multisystem inflammatory syndrome in children (MIS-C) is a rare, severe complication of COVID-19. A better knowledge of immunological, cellular, and genetic characteristics of MIS-C could help better understand the pathogenesis of the disease and contribute to identifying specific diagnostic biomarkers and develop targeted therapies. We studied 37 MIS-C children at hospital admission and 24 healthy controls analyzing serum cytokines (IFN-α, IFN-β, IFN-γ, IL-6, IL-10, IL-17A, IL-12p70 and TNF), lymphocyte populations by flow cytometry and 386 genes related to autoimmune diseases, autoinflammation and primary immunodeficiencies by NGS. MIS-C patients showed a significant increase of serum IFNγ (despite a significant reduction of activated Th1) and ILs, even if with a great heterogeneity among patients, revealing different pathways involved in MIS-C pathogenesis and suggesting that serum cytokines at admission may help to select the inflammatory pathways to target in each patient. Flow cytometry demonstrated a relevant reduction of T populations while the percentage of B cell was increased in agreement with an autoimmune pathogenesis of MIS-C. Genetic analysis identified variants in 34 genes and 83.3% of patients had at least one gene variant. Among these, 9 were mutated in more patients. Most genes are related to autoimmune diseases like ATM, NCF1, MCM4, FCN3, and DOCK8 or to autoinflammatory diseases associated to the release of IFNγ like PRF1, NOD2, and MEF. Thus, an incomplete clearance of the Sars-CoV2 during the acute phase may induce tissue damage and self-antigen exposure and genetic variants can predispose to hyper-reactive immune dysregulation events of MIS-C-syndrome. Type II IFN activation and cytokine responses (mainly IL-6 and IL-10) may cause a cytokine storm in some patients with a more severe acute phase of the disease, lymphopenia and multisystemic organ involvement. The timely identification of such patients with an immunocytometric panel might be critical for targeted therapeutic management.

Keywords: MIS-C; autoimmune diseases; autoinflammatory diseases; cytokines; flow cytometry.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Autoantigens
Autoimmune Diseases*
Biomarkers
COVID-19*
Child
Cytokines / metabolism
Guanine Nucleotide Exchange Factors
Humans
Immunologic Deficiency Syndromes*
Interleukin-10
Interleukin-17
Interleukin-6
RNA, Viral
SARS-CoV-2

Substances

Interleukin-10
Interleukin-17
Interleukin-6
RNA, Viral
Cytokines
Biomarkers
Autoantigens
DOCK8 protein, human
Guanine Nucleotide Exchange Factors

Supplementary concepts

pediatric multisystem inflammatory disease, COVID-19 related