La presencia de receptores Fc de IgG activadores en macrófagos agrava el desarrollo de aneurisma aórtico abdominal experimental

IF 1.9 Q3 PERIPHERAL VASCULAR DISEASE Clinica e Investigacion en Arteriosclerosis Pub Date : 2023-07-01 DOI:10.1016/j.arteri.2022.12.004
Laura López-Sanz , Susana Bernal , Luna Jiménez-Castilla , Marisa Pardines , Ana Hernández-García , Luis Blanco-Colio , José Luis Martín-Ventura , Carmen Gómez Guerrero
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引用次数: 1

Abstract

Introduction

Abdominal aortic aneurysm (AAA) is a multifactorial, degenerative disease characterized by progressive aortic dilation and chronic activation of inflammation, proteolytic activity, and oxidative stress in the aortic wall. The immune response triggered by antibodies against antigens present in the vascular wall participates in the formation and progression of AAA through mechanisms not completely understood. This work analyses the function of specific IgG receptors (FcγR), especially those expressed by monocytes/macrophages, in the development of experimental AAA.

Methods

In the elastase-induced AAA model, the abdominal aortas from wildtype and FcγR deficient mice with/without macrophage adoptive transfer were analysed by histology and quantitative PCR. In vitro, mouse macrophages were transfected with RNA interference of FcγRIV/CD16.2 or treated with Syk kinase inhibitor before stimulation with IgG immune complexes.

Results

Macrophage adoptive transfer in FcγR deficient mice increased the susceptibility to AAA development. Mice receiving macrophages with functional FcγR exhibited higher aortic diameter increase, higher content of macrophages and B lymphocytes, and upregulated expression of chemokine CCL2, cytokines (TNF-α and IL-17), metalloproteinase MMP2, prooxidant enzyme NADPH oxidase-2, and the isoforms FcγRIII/CD16 and FcγRIV/CD16.2. In vitro, both FcγRIV/CD16.2 gene silencing and Syk inhibition reduced cytokines and reactive oxygen species production induced by immune complexes in macrophages.

Conclusions

Activation of macrophage FcγR contributes to AAA development by inducing mediators of inflammation, proteolysis, and oxidative stress. Modulation of FcγR or effector molecules may represent a potential target for AAA treatment.

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巨噬细胞中IgG激活剂Fc受体的存在加剧了实验性腹主动脉瘤的发展
简介腹主动脉瘤(AAA)是一种多因素退行性疾病,其特征是主动脉进行性扩张和主动脉壁炎症、蛋白水解活性和氧化应激的慢性激活。由针对血管壁中存在的抗原的抗体触发的免疫反应通过尚不完全清楚的机制参与AAA的形成和进展。本工作分析了特异性IgG受体(FcγR),特别是单核细胞/巨噬细胞表达的特异性IgG接收器在实验性AAA发展中的作用。方法在弹性蛋白酶诱导的AAA模型中,通过组织学和定量PCR分析了有/无巨噬细胞过继转移的野生型和FcγR缺陷小鼠的腹部主动脉。在体外,用FcγRIV/CD16.2的RNA干扰转染小鼠巨噬细胞,或在用IgG免疫复合物刺激之前用Syk激酶抑制剂处理。结果FcγR缺陷小鼠的巨噬细胞过继转移增加了AAA发生的易感性。接受具有功能性FcγR的巨噬细胞的小鼠表现出更高的主动脉直径增加、更高的巨噬细胞和B淋巴细胞含量,并上调趋化因子CCL2、细胞因子(TNF-α和IL-17)、金属蛋白酶MMP2、促氧化酶NADPH氧化酶-2以及同种型FcγRIII/CD16和FcγRIV/CD16.2的表达。在体外,FcγRIV/CD16.2基因沉默和Syk抑制都降低了巨噬细胞中免疫复合物诱导的细胞因子和活性氧的产生。结论巨噬细胞FcγR的激活通过诱导炎症、蛋白水解和氧化应激介质参与AAA的发展。FcγR或效应分子的调节可能代表AAA治疗的潜在靶点。
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来源期刊
Clinica e Investigacion en Arteriosclerosis
Clinica e Investigacion en Arteriosclerosis PERIPHERAL VASCULAR DISEASE-
CiteScore
3.20
自引率
6.20%
发文量
44
审稿时长
40 days
期刊介绍: La publicación idónea para acceder tanto a los últimos originales de investigación como a formación médica continuada sobre la arteriosclerosis y su etiología, epidemiología, fisiopatología, diagnóstico y tratamiento. Además, es la publicación oficial de la Sociedad Española de Arteriosclerosis.
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