University Heart Center, Department of Cardiology and Angiology I, University of Freiburg and Faculty of Medicine, 55 Hugstetter St, 79106, Freiburg, Germany.
La Jolla Institute for Allergy & Immunology, Division of Inflammation Biology, 9420 Athena Circle, La Jolla, CA, 92037, USA.
Mol Metab. 2021 Nov;53:101250. doi: 10.1016/j.molmet.2021.101250. Epub 2021 May 12.
Interferon regulatory factor (IRF) 5 is a transcription factor known for promoting M1 type macrophage polarization in vitro. Given the central role of inflammatory macrophages in promoting atherosclerotic plaque progression, we hypothesize that myeloid cell-specific deletion of IRF5 is protective against atherosclerosis.
Female ApoeLysmIrf5 and ApoeIrf5 mice were fed a high-cholesterol diet for three months. Atherosclerotic plaque size and compositions as well as inflammatory gene expression were analyzed. Mechanistically, IRF5-dependent bone marrow-derived macrophage cytokine profiles were tested under M1 and M2 polarizing conditions. Mixed bone marrow chimeras were generated to determine intrinsic IRF5-dependent effects on macrophage accumulation in atherosclerotic plaques.
Myeloid cell-specific Irf5 deficiency blunted LPS/IFNγ-induced inflammatory gene expression in vitro and in the atherosclerotic aorta in vivo. While atherosclerotic lesion size was not reduced in myeloid cell-specific Irf5-deficient Apoe mice, plaque composition was favorably altered, resembling a stable plaque phenotype with reduced macrophage and lipid contents, reduced inflammatory gene expression and increased collagen deposition alongside elevated Mertk and Tgfβ expression. Irf5-deficient macrophages, when directly competing with wild type macrophages in the same mouse, were less prone to accumulate in atherosclerotic lesion, independent of monocyte recruitment. Irf5-deficient monocytes, when exposed to oxidized low density lipoprotein, were less likely to differentiate into macrophage foam cells, and Irf5-deficient macrophages proliferated less in the plaque.
Our study provides genetic evidence that selectively altering macrophage polarization induces a stable plaque phenotype in mice.
干扰素调节因子(IRF)5 是一种已知的转录因子,可促进体外 M1 型巨噬细胞极化。鉴于炎症性巨噬细胞在促进动脉粥样硬化斑块进展中的核心作用,我们假设骨髓细胞特异性缺失 IRF5 可预防动脉粥样硬化。
给雌性 ApoeLysmIrf5 和 ApoeIrf5 小鼠喂食高胆固醇饮食三个月。分析动脉粥样硬化斑块大小和组成以及炎症基因表达。在 M1 和 M2 极化条件下测试 IRF5 依赖性骨髓源性巨噬细胞细胞因子谱,以探讨其机制。生成混合骨髓嵌合体以确定巨噬细胞在动脉粥样硬化斑块中积累的固有 IRF5 依赖性效应。
骨髓细胞特异性 Irf5 缺失减弱了体外 LPS/IFNγ诱导的炎症基因表达以及体内动脉粥样硬化主动脉中的表达。虽然骨髓细胞特异性 Irf5 缺陷型 Apoe 小鼠的动脉粥样硬化病变大小没有减少,但斑块组成得到了有利的改变,类似于稳定斑块表型,表现为巨噬细胞和脂质含量减少、炎症基因表达降低、胶原沉积增加,同时 Mertk 和 Tgfβ 表达升高。当 Irf5 缺陷型巨噬细胞与同一只小鼠中的野生型巨噬细胞直接竞争时,它们在动脉粥样硬化病变中积累的倾向较小,这与单核细胞募集无关。当接触氧化低密度脂蛋白时,Irf5 缺陷型单核细胞不太可能分化为巨噬细胞泡沫细胞,并且 Irf5 缺陷型巨噬细胞在斑块中的增殖减少。
本研究提供了遗传证据,表明选择性改变巨噬细胞极化可诱导小鼠形成稳定的斑块表型。
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