Osteopontin Promotes Cholangiocyte Secretion of Chemokines to Support Macrophage Recruitment and Fibrosis in MASH.

IF 6 2区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Jason D Coombes, Paul P Manka, Marzena Swiderska-Syn, Danielle T Vannan, Antonio Riva, Lee C Claridge, Cynthia Moylan, Ayako Suzuki, Marco A Briones-Orta, Rasha Younis, Naoto Kitamura, Svenja Sydor, Shanna Bittencourt, Zhiyong Mi, Paul C Kuo, Anna Mae Diehl, Leo A van Grunsven, Shilpa Chokshi, Ali Canbay, Manal F Abdelmalek, Patricia Aspichueta, Salvatore Papa, Bertus Eksteen, Wing-Kin Syn
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引用次数: 0

Abstract

Background and aims: Osteopontin (OPN) promotes the ductular reaction and is a major driver of chronic liver disease (CLD) progression. Although CLD is characterised by the accumulation of inflammatory cells including macrophages around the peri-portal regions, the influence of OPN on recruitment is unclear. We investigated the role of OPN in cholangiocyte chemokine production and macrophage recruitment by combining in vivo, in vitro, and in silico approaches.

Methods: The effects of OPN on cholangiocyte chemokine production and macrophage migration were assessed in culture, alongside RNA-sequencing to identify genes and pathways affected by OPN depletion. Murine liver injury models were used to assess liver chemokine expression and liver macrophage/monocyte recruitment. OPN and chemokine expression were analysed in liver tissue and plasma from biopsy-proven metabolic dysfunction-associated alcoholic steatohepatitis (MASH) patients.

Results: OPN-knockdown in cholangiocytes reduced chemokine secretion. RNA-sequencing showed OPN-related effects clustered around immunity, chemotaxis and chemokine production. Macrophage exposure to cholangiocyte-conditioned media showed OPN-supported migration via chemokines chemokine (C-C motif) ligand (CCL)2, CCL5 and chemokine (C-X-C motif) ligand (CXCL)1. These effects were related to NF-κB signalling. Murine liver fibrosis was accompanied by upregulated liver OPN, CCL2, CCL5 and CXCL1 mRNA, and accumulation of liver cluster of differentiation (CD)11b/F4/80+CC chemokine receptors (CCR2)high macrophages but treatment with OPN-specific neutralising aptamers reduced fibrosis, chemokine mRNAs and accumulation of liver CD11b/F4/80+CCR2high/lymphocyte antigen 6 complexhigh inflammatory monocytes. In human MASH, liver OPN correlated with chemokines CCL2 and IL8 in association with portal injury and fibrosis. Plasma OPN, serum CCL2 and IL8 also increased with fibrosis stage.

Conclusions: OPN promotes cholangiocyte chemokine secretion and the accumulation of pro-inflammatory monocytes. These data support neutralisation of OPN as an anti-inflammatory and anti-fibrotic strategy.

骨蛋白促进胆管细胞分泌趋化因子,支持 MASH 中巨噬细胞的招募和纤维化。
背景和目的:骨化蛋白(OPN)可促进导管反应,是慢性肝病(CLD)进展的主要驱动因素。虽然 CLD 的特征是炎症细胞(包括巨噬细胞)在门静脉周围区域聚集,但 OPN 对招募的影响尚不清楚。我们结合体内、体外和硅学方法研究了 OPN 在胆管细胞趋化因子生成和巨噬细胞招募中的作用:方法:在培养过程中评估OPN对胆管细胞趋化因子产生和巨噬细胞迁移的影响,同时进行RNA测序以确定受OPN耗竭影响的基因和通路。小鼠肝损伤模型用于评估肝脏趋化因子的表达和肝脏巨噬细胞/单核细胞的募集。对活检证实的代谢功能障碍相关酒精性脂肪性肝炎(MASH)患者的肝组织和血浆中的OPN和趋化因子表达进行了分析:结果:在胆管细胞中敲除 OPN 会减少趋化因子的分泌。RNA 序列分析表明,OPN 的相关效应集中在免疫、趋化和趋化因子分泌方面。暴露于胆管细胞条件培养基的巨噬细胞显示,OPN通过趋化因子(C-C motif)配体(CCL)2、CCL5和趋化因子(C-X-C motif)配体(CXCL)1支持迁移。这些效应与 NF-κB 信号有关。小鼠肝纤维化伴随着肝脏 OPN、CCL2、CCL5 和 CXCL1 mRNA 的上调,以及肝脏分化簇(CD)11b/F4/80+CC 趋化因子受体(CCR2)高的巨噬细胞的聚集,但用 OPN 特异性中和适配体处理可减少纤维化、趋化因子 mRNA 和肝脏 CD11b/F4/80+CCR2 高/淋巴细胞抗原 6 复合物高的炎性单核细胞的聚集。在人类 MASH 中,肝脏 OPN 与趋化因子 CCL2 和 IL8 相关,与肝门损伤和纤维化有关。血浆 OPN、血清 CCL2 和 IL8 也随着纤维化阶段的增加而增加:结论:OPN 促进胆管细胞趋化因子的分泌和促炎性单核细胞的聚集。这些数据支持将中和 OPN 作为一种抗炎和抗纤维化策略。
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
Liver International
Liver International 医学-胃肠肝病学
CiteScore
13.90
自引率
4.50%
发文量
348
审稿时长
2 months
期刊介绍: Liver International promotes all aspects of the science of hepatology from basic research to applied clinical studies. Providing an international forum for the publication of high-quality original research in hepatology, it is an essential resource for everyone working on normal and abnormal structure and function in the liver and its constituent cells, including clinicians and basic scientists involved in the multi-disciplinary field of hepatology. The journal welcomes articles from all fields of hepatology, which may be published as original articles, brief definitive reports, reviews, mini-reviews, images in hepatology and letters to the Editor.
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