Novel hypermorphic variants in IRF2BP2 identified in patients with common variable immunodeficiency and autoimmunity

IF 4.5 3区 医学 Q2 IMMUNOLOGY
Manfred Anim , Georgios Sogkas , Nadezhda Camacho-Ordonez , Gunnar Schmidt , Abdulwahab Elsayed , Michele Proietti , Torsten Witte , Bodo Grimbacher , Faranaz Atschekzei
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Abstract

The interferon regulatory factor 2 binding protein 2 (IRF2BP2) is a transcriptional regulator, functioning a transcriptional corepressor by interacting with the interferon regulatory factor-2. The ubiquitous expression of IRF2BP2 by diverse cell types and tissues suggests its potential involvement in different cell signalling pathways. Variants in IRF2BP2 have been recently identified to cause familial common variable immunodeficiency (CVID) characterized by immune dysregulation.

This study investigated three rare novel variants in IRF2BP2, identified in patients with primary antibody deficiency and autoimmunity by whole exome-sequencing (WES). Following transient overexpression of EGFP-fused mutants in HEK293 cells and transfection in Jurkat cell lines, we used fluorescence microscopy, real-time PCR and Western blotting to analyze their effects on IRF2BP2 expression, subcellular localization, nuclear translocation of IRF2, and the transcriptional activation of NFκB1(p50).

We found altered IRF2BP2 mRNA and protein expression levels in the mutants compared to the wild type after IRF2BP2 overexpression. In confocal fluorescence microscopy, variants in the C-terminal RING finger domain showed an irregular aggregate formation and distribution instead of the expected nuclear localization compared to the variants in the N-terminal zinc finger domain and their wildtype counterpart. Immunoblotting revealed an impaired IRF2 and NFκB1 (p50) nuclear localization in the mutants compared to the IRF2BP2 wildtype counterpart. LPS stimulation reduced IRF2BP2 mRNA expression in the variants compared to the wild type.

Our findings significantly contribute to understanding the clinical significance of IRF2BP2 mutations in the pathogenesis of immunodeficiency and immune dysregulation. We observed impairment of the nuclear translocation of IRF2 and NFκB1 (p50) due to the upregulation of IRF2BP2, potentially affecting specific gene expressions involved in immune regulation.

在常见变异性免疫缺陷和自身免疫患者中发现 IRF2BP2 的新型高形态变异。
干扰素调节因子 2 结合蛋白 2(IRF2BP2)是一种转录调节因子,通过与干扰素调节因子-2 相互作用而发挥转录核心抑制因子的功能。IRF2BP2 在不同的细胞类型和组织中普遍表达,这表明它可能参与了不同的细胞信号通路。最近发现,IRF2BP2 的变异可导致以免疫失调为特征的家族性常见可变免疫缺陷症(CVID)。本研究调查了通过全外显子组测序(WES)在原发性抗体缺乏和自身免疫患者中发现的IRF2BP2的三个罕见新型变体。在 HEK293 细胞中瞬时过表达 EGFP 融合突变体并转染 Jurkat 细胞系后,我们使用荧光显微镜、实时 PCR 和 Western 印迹法分析了它们对 IRF2BP2 表达、亚细胞定位、IRF2 核转位和 NFκB1(p50) 转录激活的影响。我们发现,与野生型相比,IRF2BP2过表达后突变体的IRF2BP2 mRNA和蛋白表达水平发生了改变。在共聚焦荧光显微镜下,与 N 端锌指结构域的变体及其野生型相比,C 端 RING 手指结构域的变体显示出不规则的聚集体形成和分布,而不是预期的核定位。免疫印迹显示,与 IRF2BP2 野生型对应物相比,突变体的 IRF2 和 NFκB1 (p50) 核定位功能受损。与野生型相比,LPS 刺激降低了变异体中 IRF2BP2 mRNA 的表达。我们的发现大大有助于理解IRF2BP2突变在免疫缺陷和免疫失调发病机制中的临床意义。我们观察到,由于IRF2BP2的上调,IRF2和NFκB1 (p50)的核转位受损,可能会影响参与免疫调节的特定基因表达。
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来源期刊
Clinical immunology
Clinical immunology 医学-免疫学
CiteScore
12.30
自引率
1.20%
发文量
212
审稿时长
34 days
期刊介绍: Clinical Immunology publishes original research delving into the molecular and cellular foundations of immunological diseases. Additionally, the journal includes reviews covering timely subjects in basic immunology, along with case reports and letters to the editor.
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