NF-κB c-Rel is a critical regulator of TLR7-induced inflammation in psoriasis.

IF 9.7 1区 医学 Q1 MEDICINE, RESEARCH & EXPERIMENTAL
Angela Rose Liu, Nandini Sarkar, Jordan D Cress, Tristan J de Jesus, Ananya Vadlakonda, Joshua T Centore, Alexis D Griffith, Bethany Rohr, Thomas S McCormick, Kevin D Cooper, Parameswaran Ramakrishnan
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引用次数: 0

Abstract

Background: Nuclear factor kappa B (NF-κB) c-Rel is a psoriasis susceptibility locus, however mechanisms underlying c-Rel transactivation during disease are poorly understood. Inflammation in psoriasis can be triggered following Toll-like Receptor 7 (TLR7) signalling in dendritic cells (DCs), and c-Rel is a critical regulator of DC function. Here, we studied the mechanism of TLR7-induced c-Rel-mediated inflammation in DCs.

Methods: The overall expression of c-Rel was analysed in skin sections from patients with psoriasis in human transcriptomics datasets as well as the imiquimod-induced psoriasis mouse model. The function of c-Rel in DCs following TLR7 stimulation was determined by c-Rel CRISPR/Cas9 knockout DC2.4 immortalised cells and primary bone marrow derived dendritic cells from c-Rel knockout C57BL6/J mice.

Findings: c-Rel is highly expressed in lesional skin of patients with psoriasis and TLR7-induced psoriatic lesions in mice. c-Rel deficiency protected mice from the disease, and specifically compromised TLR7-induced, and not TLR9- or TLR3-induced, inflammation in dendritic cells. Mechanistically, c-Rel deficiency disrupted activating NF-κB dimers and allowed binding of inhibitory NF-κB homodimers to the IL-1β and IL-6 promoters thus inhibiting their expression. This functionally compromises the ability of c-Rel deficient DCs to induce Th17 polarisation, which is critical in psoriasis pathogenesis.

Interpretation: Our findings reveal that c-Rel is a key regulator of TLR7-mediated dendritic cell-dependent inflammation, and that targeting c-Rel-dependent signalling could prove an effective strategy to dampen excessive inflammation in TLR7-related skin inflammation.

Funding: A complete list of funding sources that contributed to this study can be found in the Acknowledgements section.

NF-κB c-Rel是银屑病中TLR7诱导的炎症的关键调节因子。
背景:核因子卡巴B(NF-κB)c-Rel是银屑病的易感基因位点,但人们对c-Rel在发病过程中的转录激活机制知之甚少。树突状细胞(DC)中的Toll样受体7(TLR7)信号可诱发银屑病炎症,而c-Rel是DC功能的关键调节因子。在此,我们研究了TLR7诱导的c-Rel介导的DC炎症机制:方法:我们分析了人类转录组学数据集中银屑病患者皮肤切片以及咪喹莫特诱导的银屑病小鼠模型中 c-Rel 的总体表达。c-Rel CRISPR/Cas9 基因敲除的 DC2.4 永生细胞和来自 c-Rel 基因敲除的 C57BL6/J 小鼠的原始骨髓衍生树突状细胞测定了 TLR7 刺激后 DC 中 c-Rel 的功能。研究结果:c-Rel在银屑病患者的皮损皮肤和TLR7诱导的小鼠银屑病皮损中高表达。c-Rel缺失可保护小鼠免受银屑病的侵袭,并特别损害TLR7诱导的树突状细胞炎症,而不是TLR9或TLR3诱导的树突状细胞炎症。从机理上讲,c-Rel 缺乏会破坏激活性 NF-κB 二聚体,使抑制性 NF-κB 同源二聚体与 IL-1β 和 IL-6 启动子结合,从而抑制它们的表达。这在功能上损害了缺乏c-Rel的DC诱导Th17极化的能力,而Th17极化在银屑病发病机制中至关重要:我们的研究结果表明,c-Rel是TLR7介导的树突状细胞依赖性炎症的关键调节因子,靶向c-Rel依赖性信号可能被证明是抑制TLR7相关皮肤炎症中过度炎症的有效策略:对本研究有贡献的资金来源的完整列表请参见致谢部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
EBioMedicine
EBioMedicine Biochemistry, Genetics and Molecular Biology-General Biochemistry,Genetics and Molecular Biology
CiteScore
17.70
自引率
0.90%
发文量
579
审稿时长
5 weeks
期刊介绍: eBioMedicine is a comprehensive biomedical research journal that covers a wide range of studies that are relevant to human health. Our focus is on original research that explores the fundamental factors influencing human health and disease, including the discovery of new therapeutic targets and treatments, the identification of biomarkers and diagnostic tools, and the investigation and modification of disease pathways and mechanisms. We welcome studies from any biomedical discipline that contribute to our understanding of disease and aim to improve human health.
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