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核因子红细胞 2 相关因子调节烧伤和吸入性损伤后全身和肺屏障功能及免疫编程。

NUCLEAR FACTOR-ERYTHROID-2-RELATED FACTOR REGULATES SYSTEMIC AND PULMONARY BARRIER FUNCTION AND IMMUNE PROGRAMMING AFTER BURN AND INHALATION INJURY.

机构信息

Department of Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, NC.

Department of Surgery, University of North Carolina at Chapel Hill, Chapel Hill, NC.

出版信息

Shock. 2023 Feb 1;59(2):300-310. doi: 10.1097/SHK.0000000000002022. Epub 2022 Nov 3.

DOI:10.1097/SHK.0000000000002022
PMID:36730842
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9957943/
Abstract

Major burn injury is associated with systemic hyperinflammatory and oxidative stresses that encompass the wound, vascular, and pulmonary systems that contribute to complications and poor outcomes. These stresses are exacerbated if there is a combined burn and inhalation (B+I) injury, which leads to increases in morbidity and mortality. Nuclear factor-erythroid-2-related factor (NRF2) is a transcription factor that functions to maintain homeostasis during stress, in part by modulating inflammation and oxidative injury. We hypothesized that the NRF2-mediated homeostasis after burn alone and combined B-I injury is insufficient, but that pharmacological activation of the NRF2 pathway has the potential to reduce/reverse acute hyper inflammatory responses. We found that, after burn and B+I injury, Nrf2 -/- mice have higher mortality and exhibit greater pulmonary edema, vascular permeability, and exacerbated pulmonary and systemic proinflammatory responses compared with injured wild-type (WT) controls. Transcriptome analysis of lung tissue revealed specific Nrf2 -dependent dysregulated immune pathways after injury. In WT mice, we observed that B+I injury induces cytosolic, but not nuclear, accumulation of NRF2 protein in the lung microenvironment compared with sham-injured controls. Bardoxolone methyl (CDDO-Me)-containing microparticles (CDDO-MPs) were developed that allow for dilution in saline and stable release of CDDO-Me. When delivered intraperitoneally into mice 1 hour after B+I injury, CDDO-MPs significantly reduced mortality and cytokine dysfunction compared with untreated B-I animals. These data implicate the role of NRF2 regulation of pulmonary and systemic immune dysfunction after burn and B+I injury, and also a deficiency in controlling immune dysregulation. Selectively activating the NRF2 pathway may improve clinical outcomes in burn and B+I patients.

摘要

严重烧伤与全身性炎症和氧化应激有关,这些应激涵盖了伤口、血管和肺部系统,导致并发症和不良预后。如果同时存在烧伤和吸入性损伤(B+I),这些应激会加剧,导致发病率和死亡率增加。核因子-红细胞 2 相关因子(NRF2)是一种转录因子,在应激时通过调节炎症和氧化损伤来维持内稳态。我们假设,烧伤单独和合并 B+I 损伤后的 NRF2 介导的内稳态不足,但 NRF2 通路的药理学激活有可能减轻/逆转急性炎症反应。我们发现,烧伤和 B+I 损伤后,Nrf2 -/- 小鼠的死亡率更高,肺水肿、血管通透性和急性全身炎症反应更严重,与受伤的野生型(WT)对照相比。肺组织的转录组分析显示,损伤后存在特定的 Nrf2 依赖性失调免疫途径。在 WT 小鼠中,我们观察到与假伤对照相比,B+I 损伤诱导肺微环境中 NRF2 蛋白的细胞质而非核积累。开发了含有 Bardoxolone methyl(CDDO-Me)的微粒(CDDO-MPs),可在生理盐水中稀释并稳定释放 CDDO-Me。在 B+I 损伤后 1 小时通过腹腔内给药,CDDO-MPs 与未治疗的 B-I 动物相比,显著降低死亡率和细胞因子功能障碍。这些数据表明,NRF2 调节烧伤和 B+I 损伤后肺和全身免疫功能障碍的作用,以及控制免疫失调的缺陷。选择性激活 NRF2 通路可能改善烧伤和 B+I 患者的临床预后。

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