依赖 PAD4 的中性粒细胞胞外捕获器的形成对克罗恩病肠纤维化早期发展的影响

Journal of Crohn's & colitis Pub Date : 2024-08-10 DOI:10.1093/ecco-jcc/jjae121

Gabriele Dragoni, Bo-Jun Ke, Lucia Picariello, Saeed Abdurahiman, Elisabetta Ceni, Francesca Biscu, Tommaso Mello, Simone Polvani, Tommaso Innocenti, Valérie Spalart, Stefano Milani, Andre D'Hoore, Gabriele Bislenghi, Stefano Scaringi, Bram Verstockt, Gert De Hertogh, Kimberly Martinod, Andrea Galli, Gianluca Matteoli, Séverine Vermeire

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引用次数: 0

摘要

背景和目的：在炎症的早期阶段，活化的中性粒细胞以 PAD4 依赖性方式挤出中性粒细胞胞外捕获物（NETs），从而加重组织损伤和重塑。在这项研究中，我们调查了克罗恩病（CD）中中性粒细胞胞外捕获物的潜在促纤维化特性和信号传导：方法：通过多重免疫荧光染色法在克罗恩病患者切除的回肠上标记 NETs 和活化的成纤维细胞。方法：通过多重免疫荧光染色对 CD 患者切除的回肠上的 NETs 和活化的成纤维细胞进行标记，并通过大量 RNA 序列分析 NETs 处理过的人原代肠成纤维细胞，以揭示细胞信号通路，同时通过高通量成像评估胶原蛋白的生成和迁移活性。通过用 NF-kB-luciferase 报告质粒转染 CCD-18Co 成纤维细胞，并加入 C29 以阻断 TLR2 信号传导，从而评估了 TLR2/NF-kB 通路。利用慢性 DSS 小鼠模型来确定中性粒细胞（MRP8-Cre，Pad4fl/fl）中 PAD4 缺失的特殊作用：结果：免疫荧光显示，CD 患者回肠溃疡中的嗜中性粒细胞和活化的成纤维细胞在空间上共定位。转录组分析显示，NETs处理的成纤维细胞中促纤维化基因上调，TLR信号通路被激活。NETs处理可诱导成纤维细胞增殖、降低迁移能力并增加胶原释放。转染实验表明，NETs 会显著增加 NF-kB 的表达，而 C29 则会降低胶原蛋白的表达和释放。同样，在患有慢性 DSS 结肠炎的 MRP8-Cre、Pad4fl/fl 小鼠结肠中观察到胶原蛋白含量明显减少：结论：NET 可通过 TLR2/NF-kB 通路成为肠道内成纤维细胞病理激活的初始刺激物。鉴于NETs早期参与炎症，抑制PAD4可能是调节CD炎症和纤维形成的一种策略。

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The Impact of PAD4-dependent Neutrophil Extracellular Trap Formation on the Early Development of Intestinal Fibrosis in Crohn's Disease.

Background and aims: During early phases of inflammation, activated neutrophils extrude neutrophil extracellular traps (NETs) in a PAD4-dependent manner, aggravating tissue injury and remodelling. In this study, we investigated the potential pro-fibrotic properties and signalling of NETs in Crohn's disease (CD).

Methods: NETs and activated fibroblasts were labelled on resected ileum from CD patients by multiplex immunofluorescence staining. NETs-treated human primary intestinal fibroblasts were analysed by bulk RNA-sequencing to uncover cell signalling pathways, and by high-throughput imaging to assess collagen production and migratory activity. Consequentially, TLR2/NF-kB pathway was evaluated by transfection of CCD-18Co fibroblasts with NF-kB-luciferase reporter plasmid, incorporating C29 to block TLR2 signalling. A chronic DSS mouse model was used to define the specific role of PAD4 deletion in neutrophils (MRP8-Cre, Pad4fl/fl).

Results: Immunofluorescence showed spatial co-localisation of NETs and activated fibroblasts in ileal ulcerations of CD patients. Transcriptomic analysis revealed upregulation of pro-fibrotic genes and activation of TLR-signalling pathways in NETs-treated fibroblasts. NETs treatment induced fibroblast proliferation, diminished migratory capability, and increased collagen release. Transfection experiments indicated a substantial increase in NF-kB expression with NETs, whereas C29 led to decreased expression and release of collagen. In line, a significantly reduction in collagen content was observed in the colon of MRP8-Cre, Pad4fl/fl mice subjected to chronic DSS colitis.

Conclusions: NETs potentially serve as an initial stimulus for pathological activation of fibroblasts within the intestine via the TLR2/NF-kB pathway. Given their early involvement in inflammation, inhibition of PAD4 might offer a strategy to modulate both inflammation and fibrogenesis in CD.

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Journal of Crohn's & colitis

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