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Butyrate impairs atherogenesis by reducing plaque inflammation and vulnerability and decreasing NFκB activation

丁酸盐 炎症 CD36 化学 促炎细胞因子 巨噬细胞 肿瘤坏死因子α 内科学 内分泌学 生物 医学 生物化学 发酵 受体 体外
作者
Edenil Costa Aguilar,Alda Jusceline Leonel,Lílian Gonçalves Teixeira,A.R. Silva,Josiane F. Silva,Juliana M. Navia‐Pelaez,Luciano dos Santos Aggum Capettini,Virgı́nia S. Lemos,Robson A.S. Santos,Jacqueline I. Alvarez‐Leite
出处
期刊:Nutrition Metabolism and Cardiovascular Diseases [Elsevier BV]
卷期号:24 (6): 606-613 被引量:236
标识
DOI:10.1016/j.numecd.2014.01.002
摘要

Butyrate is a four-carbon fatty acid that presents anti-inflammatory, anti-oxidative and apoptotic properties in colon and several cell lines. Because atherosclerosis has important oxidative and inflammatory components, butyrate could reduce oxidation and inflammation, impairing atherogenesis. We evaluated the effects of butyrate supplementation of butyrate on atherosclerosis and its mechanisms of action.ApoE knockout mice were fed on chow diet or 1% butyrate-supplemented chow diet (Butyrate) for 10 weeks to assess atherosclerosis lesions area and inflammatory status. Macrophage and endothelial cells were also pretreated with butyrate (0.5 mM) for 2 h before oxLDL stimulation to study oxLDL uptake and pro and anti-inflammatory cytokine production. Butyrate reduced atherosclerosis in the aorta by 50%. In the aortic valve, butyrate reduced CCL2, VCAM1 and MMP2 productions in the lesion site, resulting in a lower migration of macrophage and increased collagen depositions in the lesion and plaque stability. When EA.hy926 cells were pretreated with butyrate, oxLDL uptake, CD36, VCAM1, CCL2 TNF, IL1β and IL6 productions were reduced, whereas IL10 production was increased. These effects were accompanied by a lower activation of NFκB due to a lower nuclear translocation of the p65 subunit.Oral butyrate is able to slow the progression of atherosclerosis by reducing adhesion and migration of macrophages and increasing plaque stability. These actions are linked to the reduction of CD36 in macrophages and endothelial cells, decreased pro-inflammatory cytokines and lower activation of NFκB all of these data support a possible role for butyrate as an atheroprotective agent.
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