BPIFA1 alleviates allergic rhinitis by regulating the NF-κB signaling pathway and Treg/Th17 balance

IF 2.4 4区 医学 Q2 RHEUMATOLOGY
Ying Yang, Shidong Li, Hongyan Xu
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引用次数: 0

Abstract

Aim

Allergic rhinitis (AR) is an allergic condition characterized by inflammation of the nasal mucosa. Bacterial permeability-increasing family member A1 (BPIFA1) exhibits anti-inflammatory properties; however, its impact on AR remains unclear. Aim of this study is to investigate the expression and function of BPIFA1 in AR and its influence on inflammation and immune regulation in a mouse model of AR induced by ovalbumin (OVA).

Methods

The expression of BPIFA1 was analyzed using quantitative real-time PCR (qRT-PCR) and immunohistochemistry (IHC). Morphological assessments of nasal mucosal tissues were conducted. Levels of inflammatory mediators in nasal lavage fluid (NALF) and serum were quantified using enzyme-linked immunosorbent assay (ELISA) kits. Protein expressions of BPIFA1, phosphorylated and total p65 (p-p65/p65), and IκBα were evaluated through Western blot analysis. The total cell counts, including epithelial cells, eosinophils, and lymphocytes in NALF, were determined using a hemocytometer. A mouse model of AR was established by OVA management.

Results

BPIFA1 expression was found to be reduced in the nasal mucosa tissues of patients with AR, suggesting a potential role in the disease's progression. We successfully developed a mouse model of AR, where BPIFA1 was similarly downregulated, indicating its possible involvement in modulating the NF-κB signaling pathway. Overexpression of BPIFA1 in this model attenuated inflammation and allergic responses by inhibiting the NF-κB pathway. Additionally, overexpression of BPIFA1 promoted the differentiation of regulatory T cells (Treg) and inhibited the differentiation of T helper 17 cells (Th17) in the NALF of AR mice, further demonstrating its regulatory impact on immune responses. The study confirmed that BPIFA1 upregulation reduced the levels of inflammatory cytokines TNF-α and IL-6, decreased infiltration of inflammatory cells, and modulated antigen-specific immunoglobulin levels and histamine in serum.

Conclusion

BPIFA1 mitigated both inflammatory and allergic responses in AR mice induced by OVA through the modulation of the NF-κB signaling pathway and the balance between regulatory T cells (Treg) and T helper 17 cells (Th17). These findings suggest that BPIFA1 could serve as a novel biomarker and therapeutic target for AR, offering potential for the development of targeted treatments to improve patient outcomes.

BPIFA1通过调节NF-κB信号通路和Treg/Th17平衡缓解过敏性鼻炎。
目的:过敏性鼻炎(AR)是一种以鼻粘膜炎症为特征的过敏性疾病。细菌渗透性增加家族成员 A1(BPIFA1)具有抗炎特性,但其对 AR 的影响仍不清楚。本研究旨在研究 BPIFA1 在卵清蛋白(OVA)诱导的 AR 小鼠模型中的表达和功能及其对炎症和免疫调节的影响:方法:采用定量实时PCR(qRT-PCR)和免疫组织化学(IHC)分析BPIFA1的表达。对鼻粘膜组织进行形态学评估。使用酶联免疫吸附试验(ELISA)试剂盒对鼻腔灌洗液(NALF)和血清中的炎症介质水平进行了定量分析。通过 Western 印迹分析评估了 BPIFA1、磷酸化 p65 和总 p65(p-p65/p65)以及 IκBα 的蛋白表达。使用血细胞计数器测定了细胞总数,包括 NALF 中的上皮细胞、嗜酸性粒细胞和淋巴细胞。通过OVA管理建立了AR小鼠模型:结果:发现BPIFA1在AR患者的鼻粘膜组织中表达减少,这表明BPIFA1在疾病的发展过程中起着潜在的作用。我们成功建立了一个 AR 小鼠模型,在该模型中,BPIFA1 也同样被下调,这表明它可能参与了 NF-κB 信号通路的调节。在该模型中,过表达 BPIFA1 可抑制 NF-κB 通路,从而减轻炎症和过敏反应。此外,在AR小鼠的NALF中,过表达BPIFA1可促进调节性T细胞(Treg)的分化,抑制T辅助17细胞(Th17)的分化,进一步证明了它对免疫反应的调节作用。研究证实,BPIFA1 的上调降低了炎性细胞因子 TNF-α 和 IL-6 的水平,减少了炎性细胞的浸润,并调节了血清中抗原特异性免疫球蛋白和组胺的水平:结论:BPIFA1通过调节NF-κB信号通路以及调节性T细胞(Treg)和T辅助17细胞(Th17)之间的平衡,减轻了OVA诱导的AR小鼠的炎症和过敏反应。这些研究结果表明,BPIFA1可作为AR的新型生物标记物和治疗靶点,为开发靶向治疗以改善患者预后提供了潜力。
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来源期刊
CiteScore
3.70
自引率
4.00%
发文量
362
审稿时长
1 months
期刊介绍: The International Journal of Rheumatic Diseases (formerly APLAR Journal of Rheumatology) is the official journal of the Asia Pacific League of Associations for Rheumatology. The Journal accepts original articles on clinical or experimental research pertinent to the rheumatic diseases, work on connective tissue diseases and other immune and allergic disorders. The acceptance criteria for all papers are the quality and originality of the research and its significance to our readership. Except where otherwise stated, manuscripts are peer reviewed by two anonymous reviewers and the Editor.
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