氧化三甲胺参与慢性自发性荨麻疹发病的机制研究

doi:10.35541/cjd.20240687

中华皮肤科杂志 ›› 2025, Vol. 58 ›› Issue (6): 515-522.doi: 10.35541/cjd.20240687

氧化三甲胺参与慢性自发性荨麻疹发病的机制研究

唐汇洋¹ 杨芷¹ 杨希¹ 姚正秋¹ 郝飞¹ 陈邦涛²

¹重庆医科大学附属第三医院皮肤整形美容中心，重庆 400110；²重庆大学附属三峡医院皮肤性病科，重庆 404000

收稿日期:2024-12-13 修回日期:2025-04-19 发布日期:2025-06-03
通讯作者: 郝飞;陈邦涛 E-mail:651588@hospital.cqmu.edu.cn; medisci@163.com
基金资助:
国家自然科学基金（8200337、82373479）；重庆英才项目（cstc2021ycjh-bgzxm0291）；重庆市医学青年拔尖人才项目（YXQN202462）；万州区博士“直通车”科研资助项目（wzstc-20220122）；博士后出站留渝经费（55012）

Mechanistic studies on the involvement of trimethylamine oxide in the pathogenesis of chronic spontaneous urticaria

Tang Huiyang¹, Yang Zhi¹, Yang Xi¹, Yao Zhengqiu¹, Hao Fei¹, Chen Bangtao²

¹Dermatology and Cosmetic Center, the Third Affiliated Hospital of Chongqing Medical University, Chongqing 400110, China; ²Department of Dermatology and Venereology, Chongqing University Three Gorges Hospital, Chongqing 404000, China

Received:2024-12-13 Revised:2025-04-19 Published:2025-06-03
Contact: Hao Fei; Chen Bangtao E-mail:651588@hospital.cqmu.edu.cn; medisci@163.com
Supported by:
National Natural Science Foundation of China （8200337, 82373479）；Excellence Program of Chongqing （cstc2021ycjh-bgzxm0291）; Medical Youth Top-talent Project in Chongqing （YXQN202462）; Doctoral Program in Wanzhou District （wzstc-20220122）; Funding for Postdoctoral Fellowships in Chongqing （55012）

摘要/Abstract

摘要： 【摘要】目的探索肠道菌群代谢物氧化三甲胺（TMAO）参与慢性自发性荨麻疹（CSU）发病的分子机制。方法选取2023年6月至2024年6月在重庆医科大学附属第三医院皮肤整形美容中心就诊的CSU患者67例，同时收集与患者年龄匹配的69名健康对照。采用酶联免疫吸附试验（ELISA）检测两组受试者血清中TMAO水平并收集CSU患者D-二聚体水平数据。在大鼠嗜碱性白血病细胞RBL-2H3中构建抗二硝基苯（DNP）IgE抗体/DNP-白蛋白（BSA）抗原（Ag）介导的细胞脱颗粒模型（IgE/Ag组），同时加不同浓度TMAO处理（IgE/Ag＋10 μmol/L TMAO组、IgE/Ag + 50 μmol/L TMAO组、IgE/Ag＋100 μmol/L TMAO组），以无任何处理的RBL-2H3为空白组；为探讨细胞外信号调节激酶（ERK）磷酸化抑制剂U0126对TMAO效应的影响，设置空白组、IgE/Ag组、IgE/Ag＋1 μmol/L U0126组、IgE/Ag + 100 μmol/L TMAO组、IgE/Ag＋100 μmol/L TMAO＋1 μmol/L U0126组；此外，在C57BL/6小鼠耳部构建抗DNP IgE抗体/DNP-BSA抗原（Ag）介导的局部过敏反应模型（IgE/Ag组），再设置空白组、IgE组、IgE/Ag + 溶剂（DMSO）组、IgE/Ag + 10 μg/μl TMAO组。采用ELISA法检测细胞培养上清液及小鼠血清中相关炎症介质表达，采用甲苯胺蓝染色观察细胞和小鼠耳组织中肥大细胞脱颗粒情况，采用伊文思蓝观察小鼠耳组织血管通透性，采用Western印迹法检测ERK磷酸化水平。两组间比较采用t检验，多组间比较采用单因素方差分析。结果 67例CSU患者血清TMAO水平显著高于69例健康对照（t = 13.27，P < 0.001）。在收集到临床检测D-二聚体水平的32例CSU患者中，血清TMAO水平与D-二聚体水平呈显著正相关（r = 0.62，P < 0.001）。RBL-2H3细胞实验中，与IgE/Ag组相比，IgE/Ag＋10 μmol/L TMAO组、IgE/Ag + 50 μmol/L TMAO组、IgE/Ag＋100 μmol/L TMAO组细胞脱颗粒率显著升高；同时，10、50、100 μmol/L TMAO可使IgE/Ag激活的RBL-2H3细胞形态逐渐变圆，50、100 μmol/L TMAO还能显著促进β氨基己糖苷酶（β-Hex）、白细胞介素6（IL-6）及肿瘤坏死因子α（TNF-α）的产生（均P < 0.01），并上调ERK磷酸化水平（P < 0.01）；IgE/Ag＋U0126组相比于IgE/Ag组，IgE/Ag＋TMAO＋U0126组相比于IgE/Ag + TMAO组细胞中ERK磷酸化水平、IL-6、TNF-α、β-Hex含量均较低（均P < 0.001）。小鼠局部过敏反应研究显示，与IgE/Ag + DMSO组相比，IgE/Ag + TMAO组小鼠耳组织中血管通透性、水肿程度和肥大细胞脱颗粒明显增加，同时ERK磷酸化水平和TNF-α表达显著升高（P < 0.05）。结论血清中升高的TMAO可能通过上调肥大细胞及皮肤组织中ERK磷酸化，促进IgE/Ag介导的细胞脱颗粒及炎症介质产生，参与CSU发病。

关键词: 慢性荨麻疹, 慢性自发性荨麻疹, 氧化三甲胺, 细胞外信号调节激酶, 磷酸化

Abstract: 【Abstract】 Objective To investigate the possible mechanisms underlying the involvement of the gut microbiota metabolite trimethylamine oxide （TMAO） in the pathogenesis of chronic spontaneous urticaria （CSU）. Methods From June 2023 to June 2024, 67 CSU patients were enrolled from the Dermatology and Cosmetic Center, the Third Affiliated Hospital of Chongqing Medical University, and 69 age-matched healthy controls were also collected at the same time. Serum TMAO levels in both groups were measured using enzyme-linked immunosorbent assay （ELISA）, and D-dimer levels were collected from the CSU patients. A degranulation model was established in rat basophilic leukemia RBL-2H3 cells using anti-DNP IgE/DNP-BSA （IgE/Ag group）; these cells were additionally grouped to be treated with different concentrations of TMAO （IgE/Ag＋10 μmol/L TMAO group, IgE/Ag + 50 μmol/L TMAO group, IgE/Ag＋100 μmol/L TMAO group）; untreated RBL-2H3 cells served as a blank control group. To investigate the effect of the extracellular signal-regulated kinase （ERK） phosphorylation inhibitor U0126 on the action of TMAO, RBL-2H3 cells were divided into another 5 groups: blank group, IgE/Ag group, IgE/Ag + 1 μmol/L U0126 group, IgE/Ag + 100 μmol/L TMAO group, and IgE/Ag + 100 μmol/L TMAO + 1 μmol/L U0126 group. In vivo, a localized allergic reaction model was established in the ears of C57BL/6 mice using anti-DNP IgE/DNP-BSA （IgE/Ag group）, and additional groups included blank group, IgE group, IgE/Ag + solvent （DMSO） group, and IgE/Ag + 10 μg/μl TMAO group. ELISA was performed to detect levels of inflammatory mediators in cell culture supernatants and mouse serum. Toluidine blue staining was employed to observe mast cell degranulation in the cell experiment and mouse ear tissue samples, Evans blue staining to assess vascular permeability in mouse ear tissue samples, and Western blot analysis to detect the ERK phosphorylation levels. The t test was used for comparisons between two groups, and one-way analysis of variance for multiple comparisons. Results Serum TMAO levels were significantly higher in the 67 CSU patients than in the 69 healthy controls （t = 13.27, P < 0.001）. Among the 32 CSU patients with available data about D-dimer, serum TMAO levels were positively correlated with D-dimer levels （r = 0.62, P < 0.001）. In RBL-2H3 cell experiments, degranulation rates were significantly higher in the IgE/Ag + 10, 50, and 100 μmol/L TMAO groups than in the IgE/Ag group; morphologically, RBL-2H3 cells treated with 10, 50, and 100 μmol/L TMAO became increasingly rounded; 50 and 100 μmol/L TMAO significantly promoted the production of β-hexosaminidase （β-Hex）, interleukin-6 （IL-6）, and tumor necrosis factor-α （TNF-α）（all P < 0.01）, and upregulated ERK phosphorylation levels （P < 0.01）; the levels of ERK phosphorylation, IL-6, TNF-α, and β-Hex were significantly lower in the IgE/Ag + U0126 group than in the IgE/Ag group, as well as lower in the IgE/Ag + TMAO + U0126 group than in the IgE/Ag + TMAO group （all P < 0.001）. In the mouse model of localized allergic reaction, the IgE/Ag + TMAO group showed increased vascular permeability, edema degree, and mast cell degranulation, as well as significantly elevated ERK phosphorylation levels and TNF-α expression in mouse ear tissues compared with the IgE/Ag + DMSO group（both P < 0.05）. Conclusion Elevated serum TMAO may participate in the pathogenesis of CSU by upregulating ERK phosphorylation levels in mast cells and skin tissues, thereby promoting IgE/Ag-mediated degranulation of effector cells and production of inflammatory mediators.

Key words: Chronic urticaria, Chronic spontaneous urticaria, Trimethylamine oxide, Extracellular regulated protein kinases, Phosphorylation

唐汇洋杨芷样希姚正秋陈邦涛郝飞. 氧化三甲胺参与慢性自发性荨麻疹发病的机制研究[J]. 中华皮肤科杂志, 2025,58(6):515-522. doi:10.35541/cjd.20240687

Tang Huiyang, Yang Zhi, Yang Xi, Yao Zhengqiu, Hao Fei, Chen Bangtao. Mechanistic studies on the involvement of trimethylamine oxide in the pathogenesis of chronic spontaneous urticaria[J]. Chinese Journal of Dermatology, 2025, 58(6): 515-522.doi:10.35541/cjd.20240687

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氧化三甲胺参与慢性自发性荨麻疹发病的机制研究

Mechanistic studies on the involvement of trimethylamine oxide in the pathogenesis of chronic spontaneous urticaria

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