A genetically modulated Toll-like receptor-tolerant phenotype in peripheral blood cells of children with multisystem inflammatory syndrome.

IF 3.6 3区医学 Q2 IMMUNOLOGY

Journal of immunology Pub Date : 2025-03-18 DOI:10.1093/jimmun/vkaf006

Rehan Khan, Weizhen Ji, Jeisac Guzman Rivera, Abhilasha Madhvi, Tracy Andrews, Benjamin Richlin, Christian Suarez, Sunanda Gaur, Uzma N Hasan, William Cuddy, Aalok R Singh, Hulya Bukulmez, David Kaelber, Yukiko Kimura, Usha Ganapathi, Ioannis E Michailidis, Rahul Ukey, Sandra Moroso-Fela, John K Kuster, Myriam Casseus, Jason Roy, Jane C Burns, Lawrence C Kleinman, Daniel B Horton, Saquib A Lakhani, Maria Laura Gennaro

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引用次数: 0

Abstract

Dysregulated innate immune responses contribute to multisystem inflammatory syndrome in children (MIS-C), characterized by gastrointestinal, mucocutaneous, and/or cardiovascular injury occurring weeks after severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) exposure. To investigate innate immune functions, we stimulated ex vivo peripheral blood cells from MIS-C patients with agonists of Toll-like receptors (TLR), key innate immune response initiators. We found severely dampened cytokine responses and elevated gene expression of negative regulators of TLR signaling. Increased plasma levels of zonulin, a gut leakage marker, were also detected. These effects were also observed in fully convalescent children months after MIS-C recovery. When we investigated the genetic background of patients in relation to TLR responsiveness, we found that cells from MIS-C children carrying rare heterozygous variants of lysosomal trafficking regulator (LYST) were less refractory to TLR stimulation and exhibited lysosomal and mitochondrial abnormalities with altered energy metabolism. Moreover, these rare LYST variant heterozygous carriers tended to exhibit unfavorable clinical laboratory indicators of inflammation, including more profound lymphopenia. The results of our observational study have several implications. First, TLR hyporesponsiveness may be associated with hyperinflammation and/or excessive or prolonged stimulation with gut-originated TLR ligands. Second, TLR hyporesponsiveness during MIS-C may be protective, since LYST variant heterozygous carriers exhibited reduced TLR hyporesponsiveness and unfavorable clinical laboratory indicators of inflammation. Thus, links may exist between genetic background, ability to establish a refractory immune state, and MIS-C clinical spectrum. Third, the possibility exists that prolonged TLR hyporesponsiveness is one of the mechanisms driving long coronavirus disease (COVID), which highlights the need to monitor long-term consequences of MIS-C.

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多系统炎症综合征患儿外周血细胞中耐受 Toll 样受体的基因调控表型。

先天免疫反应失调导致儿童多系统炎症综合征（MIS-C），其特征是在严重急性呼吸综合征冠状病毒2 （SARS-CoV-2）暴露后数周发生胃肠道、粘膜皮肤和/或心血管损伤。为了研究先天免疫功能，我们用toll样受体（TLR）激动剂刺激MIS-C患者的体外外周血细胞，TLR是关键的先天免疫反应启动剂。我们发现细胞因子反应严重抑制，TLR信号负调节因子基因表达升高。此外，还检测到肠漏标志物zonulin的血浆水平升高。在MIS-C恢复几个月后完全康复的儿童中也观察到这些影响。当我们研究与TLR反应性相关的患者遗传背景时，我们发现来自携带罕见的溶酶体运输调节因子（LYST）杂合变异体的misc儿童的细胞对TLR刺激的耐受性较低，并且表现出溶酶体和线粒体异常并改变能量代谢。此外，这些罕见的LYST变异杂合携带者往往表现出不利的炎症临床实验室指标，包括更严重的淋巴细胞减少。我们观察性研究的结果有几个含义。首先，TLR低反应性可能与过度炎症和/或过度或长时间的肠道源TLR配体刺激有关。其次，MIS-C期间TLR低反应性可能具有保护作用，因为LYST变异杂合携带者表现出TLR低反应性降低和不利的炎症临床实验室指标。因此，遗传背景、建立难耐免疫状态的能力和MIS-C临床谱之间可能存在联系。第三，长期TLR低反应性可能是导致长冠状病毒病（COVID）的机制之一，这突出了监测MIS-C长期后果的必要性。

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来源期刊

Journal of immunology 医学-免疫学

CiteScore

8.20

自引率

2.30%

发文量

495

审稿时长

1 months

期刊介绍： The JI publishes novel, peer-reviewed findings in all areas of experimental immunology, including innate and adaptive immunity, inflammation, host defense, clinical immunology, autoimmunity and more. Special sections include Cutting Edge articles, Brief Reviews and Pillars of Immunology. The JI is published by The American Association of Immunologists (AAI)