三例伴有新型 NLRC4 基因突变的自身炎症性疾病病例,以及首次报道的与自身炎症性婴儿小肠结肠炎(AIFEC)相关的 NLRC4 CARD 结构域基因突变。

IF 2.8 3区 医学 Q1 PEDIATRICS Pediatric Rheumatology Pub Date : 2024-10-18 DOI:10.1186/s12969-024-01020-z
Kosar Asna Ashari, Nima Parvaneh, Kayvan Mirnia, Mehri Ayati, Maryam Saeedi, Farhad Salehzadeh, Mohammad Shahrooei, Razieh Sangsari, Pejman Rohani, Vahid Ziaee
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引用次数: 0

摘要

背景:NOD 样受体家族含 CARD 的 4 蛋白(NLRC4)基因的功能增益(GOF)突变可诱发多种自身炎症表型。目前,我们将其分为四类:家族性寒冷自身炎症综合征(FCAS)4、自身炎症性婴儿小肠结肠炎(AIFEC)、NLRC4-巨噬细胞相关综合征(MAS)和新生儿发病多系统炎症性疾病(NOMID)。由于这种疾病的罕见性和复杂性,我们有必要描述新的病例,并重新审视我们对这种疾病的认识:我们介绍了三例具有 NLRC4-GOF 突变和 AIFEC 表型的患者。第一例患者是一名女婴,患有周期性发热、癫痫发作、高炎症指标和巨噬细胞相关综合征(MAS)。母亲和外祖母从小就有反复发烧的病史。在 NLRC4 的 CARD 域发现了一个杂合突变:c.A91C: p.Asn31His。第二例患者是一名青少年男孩,患有周期性发热、腹泻、阿弗他口腔炎、癫痫发作和中枢神经系统(CNS)血管炎。在 NLRC4 基因中发现了一个杂合突变:c.1202T > C. p. Val401Ala。第三例患者是一名患有慢性腹泻和炎症指标升高的儿童。我们在 NLRC4 基因中发现了一个杂合突变:c.390delG: p.S132Afs*21。所有突变均为首次报道的与自身炎症相关的 NLRC4 基因突变。我们在第一个和第三个病例中分别引入了CARD结构域和CARD与NBD结构域之间的新型突变。经过治疗,三名患儿的病情均得到缓解:结论:NLRC4-GOF突变可能与伴有多种症状的自身炎症有关。结论:NLRC4-GOF 基因突变可能与自身炎症有关,并伴有多种症状。鉴于该病的罕见性和发现新突变的可能性,表型与基因型之间是否存在相关性还有待深入研究。由于表现和严重程度各不相同,因此需要采取不同的治疗方法。阿达木单抗在我们的 AIFEC 病例中显示出良好的疗效。
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Three cases of autoinflammatory disease with novel NLRC4 mutations, and the first mutation reported in the CARD domain of NLRC4 associated with autoinflammatory infantile enterocolitis (AIFEC).

Background: Gain of function (GOF) mutations in NOD-like receptor family CARD-containing 4 protein (NLRC4) gene induce a wide spectrum of autoinflammatory phenotypes. Currently, we categorize them into four groups: familial cold autoinflammatory syndrome (FCAS)4, autoinflammatory infantile enterocolitis (AIFEC), NLRC4-macrophage associated syndrome (MAS), and neonatal-onset multisystem inflammatory disease (NOMID). The rarity and complexity of the disease necessitate the description of new cases and a reexamination of our understanding of the condition.

Case presentations: We present three patients with NLRC4-GOF mutations and AIFEC phenotypes. The first patient is an infant girl with periodic fever, seizure, high inflammatory markers, and an episode of macrophage associated syndrome (MAS). History of recurrent fever episodes since childhood was reported in mother and maternal grandmother. A heterozygous mutation was found in CARD domain of NLRC4: c.A91C: p.Asn31His. The second patient is an adolescent boy with periodic fever, diarrhea, aphthous stomatitis, seizure, and central nervous system (CNS) vasculitis. A heterozygous mutation was found in NLRC4 gene: c.1202T > C. p. Val401Ala. The third patient is a child with chronic diarrhea and elevated inflammatory markers. We found a heterozygous mutation in NLRC4 gene: c.390delG: p.S132Afs*21. All mutations have been reported for the first time as NLRC4 mutations associated with autoinflammation. We introduced novel mutations in the CARD domain and between CARD and NBD domain in the first and third cases, respectively. All three children are under remission following treatment.

Conclusions: NLRC4-GOF mutations can be associated with autoinflammation with diverse symptoms. Given the rarity of the disease and the possibility of new mutations being identified, the existence of a phenotype/genotype correlation has yet to be thoroughly investigated. The variety in manifestations and severity spectrum mandates a variety of treatments. Adalimumab has shown favorable outcomes in our AIFEC cases.

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来源期刊
Pediatric Rheumatology
Pediatric Rheumatology PEDIATRICS-RHEUMATOLOGY
CiteScore
4.10
自引率
8.00%
发文量
95
审稿时长
>12 weeks
期刊介绍: Pediatric Rheumatology is an open access, peer-reviewed, online journal encompassing all aspects of clinical and basic research related to pediatric rheumatology and allied subjects. The journal’s scope of diseases and syndromes include musculoskeletal pain syndromes, rheumatic fever and post-streptococcal syndromes, juvenile idiopathic arthritis, systemic lupus erythematosus, juvenile dermatomyositis, local and systemic scleroderma, Kawasaki disease, Henoch-Schonlein purpura and other vasculitides, sarcoidosis, inherited musculoskeletal syndromes, autoinflammatory syndromes, and others.
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