Neutrophil extracellular traps promote differentiation and function of fibroblasts

纤维化 肌成纤维细胞 炎症 细胞生物学 中性粒细胞胞外陷阱 自噬 细胞分化 肺纤维化 化学 细胞外基质 癌症研究 免疫学 生物 病理 医学 生物化学 细胞凋亡 基因
作者
Akrivi Chrysanthopoulou,Ioannis Mitroulis,Eirini Apostolidou,Stella Arelaki,Dimitrios Mikroulis,Theocharis Konstantinidis,Efthimios Sivridis,Μaria Κoffa,Alexandra Giatromanolaki,Dimitrios T. Boumpas,Konstantinos Ritis,Konstantinos Kambas
出处
期刊: 卷期号:233 (3): 294-307 被引量:379
标识
DOI:10.1002/path.4359
摘要

Neutrophil activation by inflammatory stimuli and the release of extracellular chromatin structures (neutrophil extracellular traps - NETs) have been implicated in inflammatory disorders. Herein, we demonstrate that NETs released by neutrophils treated either with fibrosis-related agents, such as cigarette smoke, magnesium silicate, bleomycin, or with generic NET inducers, such as phorbol 12-myristate 13-acetate, induced activation of lung fibroblasts (LFs) and differentiation into myofibroblast (MF) phenotype. Interestingly, the aforementioned agents or IL-17 (a primary initiator of inflammation/fibrosis) had no direct effect on LF activation and differentiation. MFs treated with NETs demonstrated increased connective tissue growth factor expression, collagen production, and proliferation/migration. These fibrotic effects were significantly decreased after degradation of NETs with DNase1, heparin or myeloperoxidase inhibitor, indicating the key role of NET-derived components in LF differentiation and function. Furthermore, IL-17 was expressed in NETs and promoted the fibrotic activity of differentiated LFs but not their differentiation, suggesting that priming by DNA and histones is essential for IL-17-driven fibrosis. Additionally, autophagy was identified as the orchestrator of NET formation, as shown by inhibition studies using bafilomycin A1 or wortmannin. The above findings were further supported by the detection of NETs in close proximity to alpha-smooth muscle actin (α-SMA)-expressing fibroblasts in biopsies from patients with fibrotic interstitial lung disease or from skin scar tissue. Together, these data suggest that both autophagy and NETs are involved not only in inflammation but also in the ensuing fibrosis and thus may represent potential therapeutic targets in human fibrotic diseases.
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