MacKay Children's Hospital, Taipei, Taiwan.
MacKay Junior College of Medicine, Nursing, and Management, New Taipei City, Taiwan.
Front Immunol. 2021 Feb 26;12:632890. doi: 10.3389/fimmu.2021.632890. eCollection 2021.
Coronavirus disease-19 (COVID-19) in children is usually mild but some are susceptible to a Kawasaki disease (KD)-like multisystem inflammatory syndrome in children (MIS-C) in the convalescent stage, posing a need to differentiate the phenotype, susceptibility, autoimmunity, and immunotherapy between KD and MIS-C, particularly in the upcoming mass vaccination of COVID-19. Patients with MIS-C are prone to gastrointestinal symptoms, coagulopathy, and shock in addition to atypical KD syndrome with fever, mucocutaneous lesions, lymphadenopathy, and/or cardiovascular events. MIS-C manifests KD-like symptoms that alert physicians to early recognize and adopt the KD treatment regimen for patients with MIS-C. MIS-C linked to COVID-19 teaches us infection-associated autoimmune vasculitis and vice versa. Studies on genetic susceptibility have identified certain human leukocyte antigen (HLA) locus and toll-like receptor (TLR) associated with KD and/or COVID-19. Certain HLA subtypes, such as HLA-DRB1 and HLA-MICA A4 are associated with KD. HLA-B46:01 is proposed to be the risk allele of severe COVID-19 infection, and blood group O type is a protective factor of COVID-19. The autoimmune vasculitis of KD, KD shock syndrome (KDSS), or MIS-C is mediated by a genetic variant of HLA, FcγR, and/or antibody-dependent enhancement (ADE) resulting in hyperinflammation with T helper 17 (Th17)/Treg imbalance with augmented Th17/Th1 mediators: interleukin-6 (IL-6), IL-10, inducible protein-10 (IP-10), Interferon (IFNγ), and IL-17A, and lower expression of Treg-signaling molecules, FoxP3, and transforming growth factor (TGF-β). There are certain similarities and differences in phenotypes, susceptibility, and pathogenesis of KD, KDSS, and MIS-C, by which a physician can make early protection, prevention, and precision treatment of the diseases. The evolution of immunotherapies for the diseases has shown that intravenous immunoglobulin (IVIG) alone or combined with corticosteroids is the standard treatment for KD, KDSS, and MIS-C. However, a certain portion of patients who revealed a treatment resistance to IVIG or IVIG plus corticosteroids, posing a need to early identify the immunopathogenesis, to protect hosts with genetic susceptibility, and to combat Th17/Treg imbalance by anti-cytokine or pro-Treg for reversal of the hyperinflammation and IVIG resistance. Based on physiological and pathological immunity of the diseases under genetic susceptibility and host milieu conditions, a series of sequential regimens are provided to develop a so-called "Know thyself, enemy (pathogen), and ever-victorious" strategy for the prevention and immunotherapy of KD and/or MIS-C.
儿童 2019 冠状病毒病(COVID-19)通常较轻,但部分患儿在恢复期易发生川崎病(KD)样儿童多系统炎症综合征(MIS-C),需要区分 KD 和 MIS-C 的表型、易感性、自身免疫和免疫治疗,特别是在即将大规模接种 COVID-19 疫苗的情况下。MIS-C 患者除了有发热、黏膜皮肤损伤、淋巴结病和/或心血管事件的非典型 KD 综合征外,还容易出现胃肠道症状、凝血功能障碍和休克。MIS-C 表现出 KD 样症状,这提醒医生早期识别并采用 KD 治疗方案治疗 MIS-C 患者。与 COVID-19 相关的 MIS-C 告诉我们感染相关的自身免疫性血管炎,反之亦然。关于遗传易感性的研究已经确定了某些与 KD 和/或 COVID-19 相关的人类白细胞抗原(HLA)和 Toll 样受体(TLR)。某些 HLA 亚型,如 HLA-DRB1 和 HLA-MICA A4,与 KD 相关。HLA-B46:01 被提议为严重 COVID-19 感染的风险等位基因,而血型 O 型是 COVID-19 的保护因素。KD、KD 休克综合征(KDSS)或 MIS-C 的自身免疫性血管炎由 HLA、FcγR 和/或抗体依赖性增强(ADE)的遗传变异介导,导致过度炎症,伴有辅助性 T 细胞 17(Th17)/调节性 T 细胞(Treg)失衡,增强 Th17/Th1 介质:白细胞介素-6(IL-6)、白细胞介素-10(IL-10)、诱导蛋白-10(IP-10)、干扰素(IFNγ)和白细胞介素-17A,以及 Treg 信号分子 FoxP3 和转化生长因子(TGF-β)的表达降低。KD、KDSS 和 MIS-C 的表型、易感性和发病机制存在某些相似和不同之处,医生可以通过这些相似和不同之处,早期对这些疾病进行保护、预防和精准治疗。这些疾病的免疫治疗的发展表明,静脉注射免疫球蛋白(IVIG)单独或联合皮质类固醇是 KD、KDSS 和 MIS-C 的标准治疗方法。然而,有一定比例的患者对 IVIG 或 IVIG 加皮质类固醇治疗有反应,这就需要早期识别免疫发病机制,保护具有遗传易感性的宿主,并通过抗细胞因子或促 Treg 来对抗 Th17/Treg 失衡,以逆转过度炎症和 IVIG 抵抗。基于遗传易感性和宿主环境条件下疾病的生理和病理免疫,提供了一系列连续的方案,以制定一种所谓的“知己知彼,百战不殆”的策略,用于预防和免疫治疗 KD 和/或 MIS-C。
