间充质基质细胞通过细胞外囊泡介导的 miR-186-5p/CXCL1 轴调节缓解 APAP 诱导的肝损伤。

IF 7.1 2区 医学 Q1 CELL & TISSUE ENGINEERING
Erming Zhao, Rukang Liang, Panlong Li, Di Lu, Shuhan Chen, Weikeng Tan, Yunfei Qin, Yana Zhang, Yingcai Zhang, Qi Zhang, Qiuli Liu
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引用次数: 0

摘要

背景:对乙酰氨基酚(APAP)过量是药物性肝损伤(DILI)的一个重要原因。N-乙酰半胱氨酸(NAC)是临床上使用的一线药物。然而,它很少能使 APAP 晚期毒性患者受益。间充质基质细胞(MSCs)已被证明具有治疗 DILI 的潜力。然而,间充质干细胞保护APAP诱导的肝损伤的具体机制仍不清楚:方法:腹腔注射 APAP 诱导肝损伤模型。方法:腹腔注射 APAP 诱导肝损伤模型,然后检测组织病理学、生化指标和炎性细胞因子水平,以评估间充质干细胞和间充质干细胞胞外小泡(MSC-EVs)的疗效。流式细胞术揭示了间充质干细胞和间充质干细胞胞外小泡对中性粒细胞的免疫调节作用。肝脏组织的RNA测序(RNA-Seq)用于确定间充质干细胞治疗的关键靶基因:结果:间充质干细胞和间充质干细胞-EV治疗可有效缓解APAP诱导的肝损伤并抑制中性粒细胞浸润。RNA-Seq分析和ELISA数据表明,中性粒细胞的趋化吸引因子C-X-C motif趋化因子1(CXCL1)是间充质干细胞介导的改善APAP诱导的肝损伤的关键分子。此外,中和CXCL1可减少APAP诱导的肝损伤,中性粒细胞浸润也随之减少。重要的是,我们验证了间充质干细胞-EV衍生的miR-186-5p可直接与Cxcl1的3'-UTR结合,从而抑制其在肝细胞中的表达。激动剂miR-186-5p在治疗DILI方面表现出卓越的潜力:我们的研究结果表明,间充质干细胞和间充质干细胞-EVs是缓解DILI的有效方法。靶向miR-186-5p/CXCL1轴是提高间充质干细胞和间充质干细胞-EV治疗DILI疗效的有效方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Mesenchymal stromal cells alleviate APAP-induced liver injury via extracellular vesicle-mediated regulation of the miR-186-5p/CXCL1 axis.

Background: Acetaminophen (APAP) overdose is a significant cause of drug-induced liver injury (DILI). N-acetylcysteine (NAC) is the first-line agent used in the clinic. However, it rarely benefits patients with advanced APAP toxicity. Mesenchymal stromal cells (MSCs) have demonstrated potential in treating DILI. However, the specific mechanism by which MSCs protect against APAP-induced liver injury remains unclear.

Methods: APAP was injected intraperitoneally to induce a liver injury model. We then detected histopathology, biochemical indices, and inflammatory cytokine levels to assess the efficacy of MSCs and MSC extracellular vesicles (MSC-EVs). Flow cytometry was performed to reveal the immunoregulatory effects of MSCs and MSC-EVs on the neutrophils. RNA sequencing (RNA-Seq) of liver tissues was used to identify critical target genes for MSC treatment.

Results: MSC and MSC-EV treatment effectively alleviated APAP-induced liver injury and inhibited neutrophil infiltration. RNA-Seq analysis and ELISA data indicated that C-X-C motif chemokine 1 (CXCL1), a chemoattractant for neutrophils, was a key molecule in the MSC-mediated amelioration of APAP-induced liver damage. In addition, neutralization of CXCL1 reduced APAP-induced liver damage, which was accompanied by decreased neutrophil infiltration. Importantly, we verified that MSC-EV-derived miR-186-5p directly binds to the 3'-UTR of Cxcl1 to inhibit its expression in hepatocytes. The agomir miR-186-5p showed excellent potential for the treatment of DILI.

Conclusions: Our findings suggest that MSCs and MSC-EVs are an effective approach to mitigate DILI. Targeting the miR-186-5p/CXCL1 axis is a promising approach to improve the efficacy of MSCs and MSC-EVs in the treatment of DILI.

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来源期刊
Stem Cell Research & Therapy
Stem Cell Research & Therapy CELL BIOLOGY-MEDICINE, RESEARCH & EXPERIMENTAL
CiteScore
13.20
自引率
8.00%
发文量
525
审稿时长
1 months
期刊介绍: Stem Cell Research & Therapy serves as a leading platform for translational research in stem cell therapies. This international, peer-reviewed journal publishes high-quality open-access research articles, with a focus on basic, translational, and clinical research in stem cell therapeutics and regenerative therapies. Coverage includes animal models and clinical trials. Additionally, the journal offers reviews, viewpoints, commentaries, and reports.
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