RELA单倍不全表现为克罗恩病的非典型表型。

IF 4.3 3区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY

Inflammatory Bowel Diseases Pub Date : 2025-08-28 DOI:10.1093/ibd/izaf159

Noa Tal, Liran Baram, Arne Gehlhaar, Weihong Gu, Siqi Guo, Eduardo Gonzalez Santiago, Atar Lev, Ortal Barel, Raanan Shamir, Raz Somech, Liza Konnikova, Dror S Shouval

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引用次数: 0

摘要

背景：作为NF-κB信号传导的关键组成部分，RELA的突变与免疫反应失调和炎症性疾病有关。虽然免疫缺陷表型与RELA单倍体功能不全相关的报道，但胃肠道表现仍然缺乏描述。本研究旨在描述由RELA单倍功能不全驱动的非典型克罗恩样表型患者的临床、基因组和免疫学特征。方法：全外显子组测序，Sanger测序证实结果。通过蛋白质建模、Western blotting、免疫荧光和核提取物为基础的NF-κB活化试验来评估鉴定的变异对功能的影响。免疫分析采用大规模细胞术飞行时间（CyTOF）和单细胞RNA测序（scRNA-seq）进行，并与对照组进行比较。结果：我们研究了一名17岁的男性，诊断为泛肠性克罗恩病（CD）、肛周瘘、慢性粘膜皮肤念珠菌病和慢性淋巴细胞减少症。测序鉴定出RELA的杂合错义变异（C . 587t >C, p.V196A），该变异可能会损害RELA （p65）蛋白的稳定性，通过活性降低和蛋白表达减少证实了这一点。CyTOF分析显示循环T调节细胞（Tregs）减少，粘膜Tregs缺失，高凋亡率和IFN-γ诱导水平升高，而scRNA-seq显示在多个免疫亚群中存在强大的I/II型干扰素特征。失调的粘膜相关不变T （MAIT）和细胞毒性CD4+ T细胞表现出IL23R和ADAM12的上调，进一步将RELA功能障碍与促炎T细胞反应增强和组织炎症联系起来。结论：本研究将RELA单倍体功能不全与cd样特征、Th1/Th17极化和干扰素驱动炎症联系起来，强调了非典型或难治性IBD患者基因评估的重要性。

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RELA Haploinsufficiency Manifesting as an Atypical Phenotype of Crohn's Disease.

Background: Mutations in RELA, a key component of NF-κB signaling, are associated with dysregulated immune responses and inflammatory disorders. While immunodeficiency phenotypes associated with RELA haploinsufficiency have been reported, gastrointestinal manifestations remain poorly described. This study aimed to characterize the clinical, genomic, and immunological features of a patient presenting with an atypical Crohn's-like phenotype driven by RELA haploinsufficiency.

Methods: Whole-exome sequencing was performed, and results were confirmed by Sanger sequencing. Protein modeling, Western blotting, immunofluorescence, and nuclear extract-based NF-κB activation assays were conducted to assess the functional impact of the identified variant. Immune profiling was performed using mass cytometry time of flight (CyTOF) and single-cell RNA sequencing (scRNA-seq) and compared to controls.

Results: We studied a 17-year-old male diagnosed with pan-enteric Crohn's disease (CD), perianal fistulas, chronic mucocutaneous candidiasis, and chronic lymphopenia. Sequencing identified a heterozygous missense variant in RELA (c.587T>C, p.V196A) that potentially impairs RelA (p65) protein stability, confirmed by reduced activity and diminished protein expression. CyTOF analysis revealed decreased circulating T regulatory cells (Tregs), absence of mucosal Tregs, high apoptotic rates, and elevated IFN-γ induced levels, while scRNA-seq demonstrated a robust type I/II interferon signature in multiple immune subsets. Dysregulated mucosal-associated invariant T (MAIT) and cytotoxic CD4+ T cells exhibited upregulation of IL23R and ADAM12, further linking RELA dysfunction to enhanced pro-inflammatory T cell response and tissue inflammation.

Conclusion: This study links RELA haploinsufficiency with CD-like features, Th1/Th17 polarization, and interferon-driven inflammation, emphasizing the importance of genetic evaluation in patients with atypical or refractory IBD.

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来源期刊

Inflammatory Bowel Diseases 医学-胃肠肝病学

CiteScore

9.70

自引率

6.10%

发文量

462

审稿时长

1 months

期刊介绍： Inflammatory Bowel Diseases® supports the mission of the Crohn''s & Colitis Foundation by bringing the most impactful and cutting edge clinical topics and research findings related to inflammatory bowel diseases to clinicians and researchers working in IBD and related fields. The Journal is committed to publishing on innovative topics that influence the future of clinical care, treatment, and research.