[Clinical phenotype and genotype analysis of neuroinflammation, autoinflammation, splenomegaly and anemia syndrome caused by IRAK4 gene variantion].

中华儿科杂志 Pub Date : 2025-06-02 DOI:10.3760/cma.j.cn112140-20241203-00884

S M Peng, S B X Yuan, Z X Sun, Y Zhang, W Wang, H M Song

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引用次数: 0

Abstract

Objective: To summarize the clinical and genetic features of neuroinflammation, autoinflammation, splenomegaly and anemia (NASA) syndrome and investigate the pathogenic mechanism. Methods: The clinical data of 2 patients diagnosed with NASA syndrome at Department of Pediatrics, Peking Union Medical College Hospital were retrospectively analyzed. Variants were identified by gene panel sequencing and confirmed by Sanger sequencing. The function of IRAK4 gene variants was studied in vitro. Results: Among the 2 patients, case 1 was an 8-year-old girl and case 2 was a 10-year-old boy. Both patients presented in early childhood with anemia and hepatosplenomegaly. Case 1 was also experienced recurrent seizures. Laboratory examinations showed elevated inflammatory markers and neuroimaging revealed bilateral basal ganglia calcification. In case 2, anemia and inflammation markers were well controlled after treatment with tocilizumab, while case 1 succumbed to recurrent seizures. Genetic tests verified compound heterozygous variants in IRAK4 gene: case 1 carries a nonsense variant c.592G>T (p.G198X) and a missense variant c.248A>C (p.D83A), which were respectively from the parents; case 2 carries a c.831+3A>G variant and a frameshift variant c.540delT (p.F180Lfs*26), and the former was inherited from the father and the latter from the mother. The reverse transcription and Sanger sequencing results confirmed that c.831+3A>G variant led to exon 7 skipping. In vitro studies indicated that c.592G>T, c.540delT and c.831+3A>G variants resulted in truncated interleukin-1 receptor-associated kinase-4 (IRAK4) protein while c.248A>C do not cause changes in IRAK4 protein expression level and protein length. Conclusions: NASA syndrome should be considered in children with early-onset anemia, hepatosplenomegaly, recurrent seizures, elevated inflammatory markers and intracranial calcification. IRAK4 gene variants may lead to impaired anti-inflammatory function of IRAK4 protein, contributing to the autoinflammatory phenotype.

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IRAK4基因变异引起的神经炎症、自身炎症、脾大、贫血综合征的临床表型和基因型分析。

目的：总结神经炎症、自身炎症、脾肿大及贫血（NASA）综合征的临床及遗传学特点，探讨其发病机制。方法：回顾性分析北京协和医院儿科确诊为NASA综合征的2例患者的临床资料。变异通过基因面板测序鉴定，并通过Sanger测序确认。体外研究了IRAK4基因变异的功能。结果：2例患者中，病例1为8岁女童，病例2为10岁男童。两例患者均表现为儿童早期贫血和肝脾肿大。病例1也出现反复发作。实验室检查显示炎症标志物升高，神经影像学显示双侧基底节区钙化。病例2经tocilizumab治疗后，贫血和炎症指标得到很好的控制，而病例1因复发性癫痫发作而死亡。基因检测证实IRAK4基因存在复合杂合变异体：病例1携带无义变异体C . 592g >T （p.G198X）和错义变异体C . 248a >C (p.D83A)，分别来自亲本；病例2携带c.831+3A>G变异和c.540delT移码变异（p.F180Lfs*26），前者遗传自父亲，后者遗传自母亲。逆转录和Sanger测序结果证实c.831+3A >g变异导致第7外显子跳变。体外研究表明，C . 592g >T、C . 540delt和C .831+3A>G变异导致白细胞介素-1受体相关激酶4 （IRAK4）蛋白截断，而C . 248a >C不引起IRAK4蛋白表达水平和蛋白长度的变化。结论：早发性贫血、肝脾肿大、反复发作、炎症标志物升高、颅内钙化患儿应考虑NASA综合征。IRAK4基因变异可能导致IRAK4蛋白抗炎功能受损，导致自身炎症表型。

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来源期刊

中华儿科杂志

CiteScore

1.30

自引率

0.00%

发文量

14916

期刊介绍： Chinese Journal of Pediatrics is the only high-level academic journal in the field of pediatrics in my country, supervised by the China Association for Science and Technology and sponsored by the Chinese Medical Association. It was founded in 1950. The purpose of the journal is to combine theory with practice, with emphasis on practice; to combine basic and clinical, with major clinical; to combine popularization with improvement, with emphasis on improvement. It is to promote academic exchanges in the field of pediatrics in my country; to serve the development and improvement of my country's pediatric medicine; to serve the training of pediatric medical talents in my country; and to serve the health of children in my country. Chinese Journal of Pediatrics is mainly composed of columns such as monographs, clinical research and practice, case reports, lectures, reviews, conference (symposium) minutes, clinical pathology (case) discussions, international academic exchanges, expert explanations, and new technologies.