Rare genetic variants involved in multisystem inflammatory syndrome in children: a multicenter Brazilian cohort study

被引:3
作者
Dos Reis, Barbara Carvalho Santos [1 ,2 ,3 ]
Faccion, Roberta Soares [1 ,2 ]
de Carvalho, Flavia Amendola Anisio [1 ,3 ]
Moore, Daniella Campelo Batalha Cox [4 ,5 ]
Zuma, Maria Celia Chaves [1 ,2 ]
Placa, Desiree Rodrigues [6 ,7 ]
Filgueiras, Igor Salerno [8 ]
Fonseca, Dennyson Leandro Mathias [9 ]
Cabral-Marques, Otavio [6 ,8 ,9 ,10 ,11 ,12 ]
Bonomo, Adriana Cesar [13 ,14 ,15 ,16 ]
Savino, Wilson [13 ,14 ,15 ,16 ]
Freitas, Flavia Cristina de Paula [17 ]
Faoro, Helisson [17 ]
Passetti, Fabio [17 ]
Robaina, Jaqueline Rodrigues [18 ]
de Oliveira, Felipe Rezende Caino [19 ]
Bellinat, Ana Paula Novaes [20 ]
Zeitel, Raquel de Seixas [21 ]
Salu, Margarida dos Santos [1 ,2 ,20 ]
de Oliveira, Mariana Barros Genuino [18 ]
Rodrigues-Santos, Gustavo [18 ]
Prata-Barbosa, Arnaldo [18 ,22 ]
de Vasconcelos, Zilton Farias Meira [2 ]
机构
[1] Fundacao Oswaldo Cruz FIOCRUZ, Programa Posgrad Pesquisa Aplicada Saude Crianca &, Inst Nacl Saude Mulher Crianca & Adolescente Ferna, Rio De Janeiro, RJ, Brazil
[2] Fiocruz MS, Unidade Pesquisa Clin, Lab Alta Complexidade LACIFF, IFF, Rio De Janeiro, RJ, Brazil
[3] Fiocruz MS, Dept Imunol, IFF, Rio De Janeiro, RJ, Brazil
[4] Fiocruz MS, Dept Pediat, Unidade Pacientes Graves, IFF, Rio De Janeiro, RJ, Brazil
[5] Univ Fed Fluminense, Fac Med, Niteroi, RJ, Brazil
[6] Univ Sao Paulo, Fac Ciencias Farmaceut FCF, Dept Anal Clin & Toxicol, Sao Paulo, SP, Brazil
[7] Univ Sao Paulo, Programa Posgrad Farm Fisiopatol & Toxicol, FCF, Sao Paulo, SP, Brazil
[8] Univ Sao Paulo, Inst Ciencias Biomed ICB, Dept Imunol, Sao Paulo, SP, Brazil
[9] Univ Sao Paulo, Inst Matemat & Estat IME, Programa Interunidades Posgrad Bioinformat, Sao Paulo, SP, Brazil
[10] Universal Sci Educ & Res Network USERN, Network Immun Infect Malignancy & Autoimmun NIIMA, Sao Paulo, Brazil
[11] Univ Sao Paulo, Dept Med, Div Mol Med, Sch Med, Sao Paulo, SP, Brazil
[12] Univ Sao Paulo, Lab Med Invest 29, Sch Med, Sao Paulo, Brazil
[13] Fiocruz MS, Inst Oswaldo Cruz IOC, Lab Pesquisas Timo, Rio De Janeiro, RJ, Brazil
[14] Fiocruz MS, Inst Natl Ciencia & Tecnol Neuroimunomodulacao INC, IOC, Rio De Janeiro, RJ, Brazil
[15] Fiocruz MS, Rede FAPERJ Pesquisa Neuroinflamacao, IOC, Rio De Janeiro, RJ, Brazil
[16] Fiocruz MS, Rede INOVA IOC Neuroimunomodulacao, IOC, Rio De Janeiro, RJ, Brazil
[17] Fiocruz MS, Inst Carlos Chagas ICC, Lab Regulacao Expressao Genica, Curitiba, PR, Brazil
[18] Inst Or Pesquisa & Ensino IDOR, Rio De Janeiro, Brazil
[19] Hosp Alvorada Moema, Pediat Intens Care Unit, Sao Paulo, SP, Brazil
[20] Hosp Martagao Gesteira, Pediat Intens Care Unit, Salvador, BA, Brazil
[21] Univ Estado Rio De Janeiro UERJ, Hosp Univ Pedro Ernesto HUPE, Pediat Intens Care Unit, Rio De Janeiro, Brazil
[22] Univ Fed Rio De Janeiro UFRJ, Pediat Intens Care Unit, Inst Puericultura & Pediat Martagao Gesteira IPPMG, Rio De Janeiro, Brazil
来源
FRONTIERS IN CELLULAR AND INFECTION MICROBIOLOGY | 2023年 / 13卷
基金
巴西圣保罗研究基金会;
关键词
multisystem inflammatory syndrome in children; pediatric inflammatory multisystem syndrome; coronavirus infection; mucocutaneous lymph node syndrome; Kawasaki disease; whole exome sequencing; GENOME-WIDE ASSOCIATION; KAWASAKI-DISEASE; IMMUNE DYSREGULATION; INBORN-ERRORS; MIS-C; SUSCEPTIBILITY; LOCI; A91V;
D O I
10.3389/fcimb.2023.1182257
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
IntroductionDespite the existing data on the Multisystem Inflammatory Syndrome in Children (MIS-C), the factors that determine these patients evolution remain elusive. Answers may lie, at least in part, in genetics. It is currently under investigation that MIS-C patients may have an underlying innate error of immunity (IEI), whether of monogenic, digenic, or even oligogenic origin. MethodsTo further investigate this hypothesis, 30 patients with MIS-C were submitted to whole exome sequencing. ResultsAnalyses of genes associated with MIS-C, MIS-A, severe covid-19, and Kawasaki disease identified twenty-nine patients with rare potentially damaging variants (50 variants were identified in 38 different genes), including those previously described in IFNA21 and IFIH1 genes, new variants in genes previously described in MIS-C patients (KMT2D, CFB, and PRF1), and variants in genes newly associated to MIS-C such as APOL1, TNFRSF13B, and G6PD. In addition, gene ontology enrichment pointed to the involvement of thirteen major pathways, including complement system, hematopoiesis, immune system development, and type II interferon signaling, that were not yet reported in MIS-C. DiscussionThese data strongly indicate that different gene families may favor MIS- C development. Larger cohort studies with healthy controls and other omics approaches, such as proteomics and RNAseq, will be precious to better understanding the disease dynamics.
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页数:16
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