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HIF-Overexpression and Pro-Inflammatory Priming in Human Mesenchymal Stromal Cells Improves the Healing Properties of Extracellular Vesicles in Experimental Crohn's Disease.

International journal of molecular sciences(2021)SCI 2区SCI 3区

Inst Invest Sanitaria La Fe | Univ Complutense Madrid | Hosp Dr Peset | Univ Valencia | Hosp Univ I Politecn La Fe

Cited 29|Views37
Abstract
Extracellular vesicles (EVs) derived from mesenchymal stromal cells (MSCs) have therapeutic potential in the treatment of several immune disorders, including ulcerative colitis, owing to their regenerative and immunosuppressive properties. We recently showed that MSCs engineered to overexpress hypoxia-inducible factor 1-alpha and telomerase (MSC-T-HIF) and conditioned with pro-inflammatory stimuli release EVs (EVMSC-T-HIFC) with potent immunomodulatory activity. We tested the efficacy of EVMSC-T-HIFC to repolarize M1 macrophages (Mφ1) to M2-like macrophages (Mφ2-like) by analyzing surface markers and cytokines and performing functional assays in co-culture, including efferocytosis and T-cell proliferation. We also studied the capacity of EVMSC-T-HIFC to dampen the inflammatory response of activated endothelium and modulate fibrosis. Finally, we tested the therapeutic capacity of EVMSC-T-HIFC in an acute colitis model. EVMSC-T-HIFc induced the repolarization of monocytes from Mφ1 to an Mφ2-like phenotype, which was accompanied by reduced inflammatory cytokine release. EVMSC-T-HIFc-treated Mφ1 had similar effects of immunosuppression on activated peripheral blood mononuclear cells (PBMC) as Mφ2, and reduced the adhesion of PBMCs to activated endothelium. EVMSC-T-HIFc also prevented myofibroblast differentiation of TGF-β-treated fibroblasts. Finally, administration of EVMSC-T-HIFc promoted healing in a TNBS-induced mouse colitis model in terms of preserving colon length and intestinal mucosa architecture and altering the ratio of Mφ1/ Mφ2 infiltration. In conclusion, EVMSC-T-HIFC have effective anti-inflammatory properties, making them potential therapeutic agents in cell free-based therapies for the treatment of Crohn's disease and likely other immune-mediated inflammatory diseases.
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mesenchymal stromal cells,extracellular vesicles,hypoxia-inducible factor 1-alpha,immunomodulation,macrophage repolarization,Crohn's disease
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要点】:研究揭示通过过表达HIF-1α和炎症预处理的人间充质干细胞来源的外泌体(EVMSC-T-HIFC)具有改善实验性克罗恩病愈合特性的作用。

方法】:通过基因工程技术使人间充质干细胞过表达低氧诱导因子1α和端粒酶,并经炎症刺激处理,从而释放具有免疫调节活性的外泌体。

实验】:在共培养实验中,通过分析表面标记物和细胞因子以及进行功能检测(包括吞噬作用和T细胞增殖),研究了EVMSC-T-HIFC对M1型巨噬细胞(Mφ1)的再极化作用。同时评估了EVMSC-T-HIFC对活化内皮炎症反应的抑制能力和对纤维化的调节作用。最后,在TNBS诱导的急性结肠炎模型中测试了EVMSC-T-HIFC的治疗效果,结果显示EVMSC-T-HIFC能够促进结肠长度和肠道黏膜结构的保持,并改变Mφ1/Mφ2的浸润比例。