Loss of MALT1 Function in a Patient With Combined Immunodeficiency: a Novel Pathogenic Variant and Immunological Insights.

IF 5.7 2区医学 Q1 IMMUNOLOGY

Journal of Clinical Immunology Pub Date : 2025-08-01 DOI:10.1007/s10875-025-01921-y

Zhirui Tian, Ran Chen, Yanjun Jia, Jinqiu Jiang, Rongxin Dai, Yunfei An, Xuemei Tang, Xiaodong Zhao, Lina Zhou

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Abstract

Background and objectives: Germline pathogenic variants in the mucosa-associated lymphoid tissue lymphoma translocation gene 1 (MALT1) encodes a caspase-like protease that plays a crucial role in the caspase recruitment domain (CARD)-B-cell lymphoma 10 (BCL10)-MALT1 (CBM) complex. This complex mediates the activation of nuclear factor-kB (NF-kB) pathway and are associated with diverse human diseases including combine immunodeficiency (CID), lymphoproliferation and others. This study aimed to determine the underlying cause of immune deficiency and immune dysregulation in a patient presented with recurrent respiratory infections, aphthous ulcers, dermatitis, chronic diarrhea, failure to thrive and early death.

Methods: Clinical and laboratory records were reviewed. Patients underwent next-generation sequencing (NGS), and analysis of genomic DNA was performed on the patient and her parents. Lymphocyte subsets, MALT1 expression and NF-kB signaling was evaluated by flow cytometry, RT-PCR and immunoblotting.

Results: The patient carried a novel pathogenic biallelic loss-of-function variant in MALT1 (c.1411G > A; p.D471N) located in the caspase-like domain, leading to severely reduced MALT1 protein expression. Impaired CBM-mediated NF-κB activation was confirmed by reduced phosphorylation of the p65 subunit, resulting in deficient production of IL-2 and TNF-α. This functional defect caused lower Tfr and Treg cells, a normal proportion of Tfh cells, with higher expression of activation markers PD-1 and ICOS. The patient displayed low NK cell and B cell counts, together with a developmental block at the transitional B cell stage. Additionally, the proportion of marginal zone-like B cells (MZB-like) was markedly decreased, indicating impaired B cell differentiation.

Conclusions: Human MALT1 deficiency causes profound CID by impairing CBM-mediated NF-kB signaling and MALT1-paracaspase activity. Consistent with the reported variants located in the caspase-like domain, our patient presented with an inflammatory phenotype, supporting the notion that the MALT1 D471N mutation phenocopies a partial loss of both MALT1 scaffolding function and paracaspase activity. Prompt hematopoietic stem cell transplantation (HSCT) is highly recommended as an effective therapy for MALT1 deficiency.

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合并免疫缺陷患者MALT1功能丧失：一种新的致病变异和免疫学见解。

背景和目的：黏膜相关淋巴组织淋巴瘤易位基因1 （MALT1）的种系致病变异编码一种caspase样蛋白酶，该蛋白酶在caspase募集结构域(CARD)- b细胞淋巴瘤10 (BCL10)-MALT1 （CBM）复合物中起关键作用。该复合物介导核因子- kb （NF-kB）通路的激活，并与多种人类疾病相关，包括联合免疫缺陷（CID）、淋巴细胞增殖等。本研究旨在确定出现复发性呼吸道感染、口腔溃疡、皮炎、慢性腹泻、发育不良和过早死亡的患者免疫缺陷和免疫失调的潜在原因。方法：回顾临床和实验室记录。患者接受了下一代测序（NGS），并对患者及其父母进行了基因组DNA分析。通过流式细胞术、RT-PCR和免疫印迹检测淋巴细胞亚群、MALT1表达和NF-kB信号传导。结果：患者携带MALT1 (c.1411G > a；p.D471N)位于caspase样结构域，导致MALT1蛋白表达严重降低。cbm介导的NF-κB活化受损通过p65亚基磷酸化降低证实，导致IL-2和TNF-α的产生不足。这种功能缺陷导致Tfh细胞中正常比例的Tfr和Treg细胞较低，激活标志物PD-1和ICOS表达较高。患者表现为NK细胞和B细胞计数低，同时在过渡性B细胞阶段出现发育阻滞。此外，边缘带样B细胞（MZB-like）比例明显减少，表明B细胞分化受损。结论：人类MALT1缺乏通过损害cbm介导的NF-kB信号和MALT1副半乳糖酶活性而导致严重的CID。与报道的位于caspase样结构域的变异一致，我们的患者表现出炎症表型，支持MALT1 D471N突变表型的概念，即MALT1支架功能和副caspase活性的部分丧失。及时造血干细胞移植（HSCT）被强烈推荐为治疗MALT1缺乏症的有效方法。

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来源期刊

Journal of Clinical Immunology 医学-免疫学

CiteScore

12.20

自引率

9.90%

发文量

218

审稿时长

2 months

期刊介绍： The Journal of Clinical Immunology publishes impactful papers in the realm of human immunology, delving into the diagnosis, pathogenesis, prognosis, or treatment of human diseases. The journal places particular emphasis on primary immunodeficiencies and related diseases, encompassing inborn errors of immunity in a broad sense, their underlying genotypes, and diverse phenotypes. These phenotypes include infection, malignancy, allergy, auto-inflammation, and autoimmunity. We welcome a broad spectrum of studies in this domain, spanning genetic discovery, clinical description, immunologic assessment, diagnostic approaches, prognosis evaluation, and treatment interventions. Case reports are considered if they are genuinely original and accompanied by a concise review of the relevant medical literature, illustrating how the novel case study advances the field. The instructions to authors provide detailed guidance on the four categories of papers accepted by the journal.