Division of Cardiology (Marc and Ruti Bell Program in Vascular Biology), Department of Medicine, New York University School of Medicine, New York, New York, United States of America.
PLoS One. 2011;6(12):e28534. doi: 10.1371/journal.pone.0028534. Epub 2011 Dec 6.
HMG-CoA reductase inhibitors (statins) decrease atherosclerosis by lowering low-density-lipoprotein cholesterol. Statins are also thought to have additional anti-atherogenic properties, yet defining these non-conventional modes of statin action remains incomplete. We have previously developed a novel mouse transplant model of atherosclerosis regression in which aortic segments from diseased donors are placed into normolipidemic recipients. With this model, we demonstrated the rapid loss of CD68+ cells (mainly macrophages) in plaques through the induction of a chemokine receptor CCR7-dependent emigration process. Because the human and mouse CCR7 promoter contain Sterol Response Elements (SREs), we hypothesized that Sterol Regulatory Element Binding Proteins (SREBPs) are involved in increasing CCR7 expression and through this mechanism, statins would promote CD68+ cell emigration from plaques. We examined whether statin activation of the SREBP pathway in vivo would induce CCR7 expression and promote macrophage emigration from plaques. We found that western diet-fed apoE(-/-) mice treated with either atorvastatin or rosuvastatin led to a substantial reduction in the CD68+ cell content in the plaques despite continued hyperlipidemia. We also observed a significant increase in CCR7 mRNA in CD68+ cells from both the atorvastatin and rosuvastatin treated mice associated with emigration of CD68+ cells from plaques. Importantly, CCR7(-/-)/apoE(-/-) double knockout mice failed to display a reduction in CD68+ cell content upon statin treatment. Statins also affected the recruitment of transcriptional regulatory proteins and the organization of the chromatin at the CCR7 promoter to increase the transcriptional activity. Statins promote the beneficial remodeling of plaques in diseased mouse arteries through the stimulation of the CCR7 emigration pathway in macrophages. Therefore, statins may exhibit some of their clinical benefits by not only retarding the progression of atherosclerosis, but also accelerating its regression.
羟甲基戊二酰辅酶 A 还原酶抑制剂(他汀类药物)通过降低低密度脂蛋白胆固醇来减少动脉粥样硬化。他汀类药物也被认为具有额外的抗动脉粥样硬化特性,但定义这些非传统的他汀类药物作用模式仍不完整。我们之前开发了一种新的动脉粥样硬化消退的小鼠移植模型,其中来自患病供体的主动脉段被放置在低脂血症的受体内。使用这种模型,我们证明了通过诱导趋化因子受体 CCR7 依赖性迁移过程,斑块中 CD68+细胞(主要是巨噬细胞)迅速丢失。由于人和小鼠的 CCR7 启动子含有固醇反应元件(SREs),我们假设固醇调节元件结合蛋白(SREBPs)参与增加 CCR7 表达,并且通过这种机制,他汀类药物会促进 CD68+细胞从斑块中迁移。我们研究了他汀类药物在体内激活 SREBP 途径是否会诱导 CCR7 表达并促进巨噬细胞从斑块中迁移。我们发现,即使继续存在高脂血症,用阿托伐他汀或罗苏伐他汀治疗的西方饮食喂养的 apoE(-/-) 小鼠,斑块中的 CD68+细胞含量也会显著减少。我们还观察到,阿托伐他汀和罗苏伐他汀治疗的小鼠的 CD68+细胞中的 CCR7 mRNA 显著增加,与 CD68+细胞从斑块中的迁移有关。重要的是,CCR7(-/-)/apoE(-/-) 双敲除小鼠在他汀类药物治疗后未能显示 CD68+细胞含量减少。他汀类药物还通过刺激巨噬细胞中 CCR7 迁移途径来影响转录调节蛋白的募集和染色质在 CCR7 启动子上的组织,从而增加转录活性。他汀类药物通过刺激 CCR7 迁移途径促进患病小鼠动脉中斑块的有益重塑,从而发挥其临床益处。因此,他汀类药物不仅可以延缓动脉粥样硬化的进展,还可以加速其消退,从而发挥一些临床益处。
Zotero 插件
