TNF-α promotes CXCL-1/8 production in keratinocytes by downregulating galectin-3 through NF-κB and hsa-miR-27a-3p pathway to contribute psoriasis development.

IF 2.9 4区 医学 Q3 IMMUNOLOGY
Xiao-Nan Qiu, Dan Hong, Zhen-Rui Shi, Si-Yao Lu, Yu-Xian Lai, Yan-Ling Ren, Xiu-Ting Liu, Chi-Peng Guo, Guo-Zhen Tan, Liang-Chun Wang
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引用次数: 0

Abstract

Objective: Treatment with TNF-α inhibitors improve psoriasis with minimize/minor neutrophils infiltration and CXCL-1/8 expression in psoriatic lesions. However, the fine mechanism of TNF-α initiating psoriatic inflammation by tuning keratinocytes is unclear. Our previous research identified the deficiency of intracellular galectin-3 was sufficient to promote psoriasis inflammation characterized by neutrophil accumulation. This study aims to investigate whether TNF-α participated in psoriasis development through dysregulating galectin-3 expression.

Methods: mRNA levels were assessed through quantitative real-time PCR. Flow cytometry was used to detect cell cycle/apoptosis. Western blot was used to evaluate the activation of the NF-κB signaling pathway. HE staining and immunochemistry were used to detect epidermal thickness and MPO expression, respectively. Specific small interfering RNA (siRNA) was used to knock down hsa-miR-27a-3p while plasmids transfection was used to overexpress galectin-3. Further, the multiMiR R package was utilized to predict microRNA-target interaction.

Results and discussion: We found that TNF-α stimulation altered cell proliferation and differentiation and promoted the production of psoriasis-related inflammatory mediators along with the inhibition of galectin-3 expression in keratinocytes. Supplement of galectin-3 could counteract the rise of CXCL-1/8 but not the other phenotypes of keratinocytes induced by TNF-α. Mechanistically, inhibition of the NF-κB signaling pathway could counteract the decrease of galectin-3 and the increase of hsa-miR-27a-3p expression whereas silence of hsa-miR-27a-3p could counteract the decrease of galectin-3 expression induced by TNF-α treatment in keratinocytes. Intradermal injection of murine anti-CXCL-2 antibody greatly alleviated imiquimod-induced psoriasis-like dermatitis.

Conclusion: TNF-α initiates psoriatic inflammation by increasing CXCL-1/8 in keratinocytes mediated by the axis of NF-κB-hsa-miR-27a-3p-galectin-3 pathway.

TNF-α通过NF-κB和hsa-miR-27a-3p通路下调半凝集素-3,促进角化细胞中CXCL-1/8的产生,促进银屑病的发展。
目的:TNF-α抑制剂治疗银屑病可改善银屑病病变中中性粒细胞浸润及CXCL-1/8表达。然而,TNF-α通过调节角质形成细胞引发银屑病炎症的精细机制尚不清楚。我们之前的研究发现,细胞内半乳糖凝集素-3的缺乏足以促进以中性粒细胞积累为特征的银屑病炎症。本研究旨在探讨TNF-α是否通过半凝集素-3表达失调参与银屑病的发展。方法:采用实时荧光定量PCR法检测各组mRNA水平。流式细胞术检测细胞周期/凋亡。Western blot检测NF-κB信号通路的激活情况。HE染色和免疫化学分别检测表皮厚度和MPO表达。用特异性小干扰RNA (siRNA)敲低hsa-miR-27a-3p,用质粒转染过表达半乳糖凝集素-3。此外,利用multiMiR R包预测microrna与靶标的相互作用。结果和讨论:我们发现TNF-α刺激改变了细胞增殖和分化,促进了银屑病相关炎症介质的产生,同时抑制了角化细胞中半凝集素-3的表达。补充半乳糖凝集素-3可抑制TNF-α诱导的角质形成细胞CXCL-1/8的升高,但对其他表型无抑制作用。在机制上,抑制NF-κB信号通路可以抵消半乳糖凝集素-3的降低和hsa-miR-27a-3p表达的增加,而hsa-miR-27a-3p的沉默可以抵消TNF-α在角质形成细胞中引起的半乳糖凝集素-3表达的降低。皮内注射小鼠抗cxcl -2抗体可显著减轻吡喹莫德诱导的银屑病样皮炎。结论:TNF-α通过NF-κB-hsa-miR-27a-3p-galectin-3通路轴介导角质形成细胞中CXCL-1/8升高引发银屑病炎症。
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来源期刊
CiteScore
5.40
自引率
0.00%
发文量
133
审稿时长
4-8 weeks
期刊介绍: The journal Immunopharmacology and Immunotoxicology is devoted to pre-clinical and clinical drug discovery and development targeting the immune system. Research related to the immunoregulatory effects of various compounds, including small-molecule drugs and biologics, on immunocompetent cells and immune responses, as well as the immunotoxicity exerted by xenobiotics and drugs. Only research that describe the mechanisms of specific compounds (not extracts) is of interest to the journal. The journal will prioritise preclinical and clinical studies on immunotherapy of disorders such as chronic inflammation, allergy, autoimmunity, cancer etc. The effects of small-drugs, vaccines and biologics against central immunological targets as well as cell-based therapy, including dendritic cell therapy, T cell adoptive transfer and stem cell therapy, are topics of particular interest. Publications pointing towards potential new drug targets within the immune system or novel technology for immunopharmacological drug development are also welcome. With an immunoscience focus on drug development, immunotherapy and toxicology, the journal will cover areas such as infection, allergy, inflammation, tumor immunology, degenerative disorders, immunodeficiencies, neurology, atherosclerosis and more. Immunopharmacology and Immunotoxicology will accept original manuscripts, brief communications, commentaries, mini-reviews, reviews, clinical trials and clinical cases, on the condition that the results reported are based on original, clinical, or basic research that has not been published elsewhere in any journal in any language (except in abstract form relating to paper communicated to scientific meetings and symposiums).
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