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小鼠模型中晚期动脉粥样硬化斑块的进展与破裂

Progression and disruption of advanced atherosclerotic plaques in murine models.

作者信息

Rosenfeld Michael E, Averill Michelle M, Bennett Brian J, Schwartz Stephen M

机构信息

Department of Environmental and Occupational Health Sciences, University of Washington, Seattle, WA 98109, USA.

出版信息

Curr Drug Targets. 2008 Mar;9(3):210-6. doi: 10.2174/138945008783755575.

Abstract

The innominate artery is a predilection site for atherosclerotic lesion formation in hyperlipidemic mice. The lesions at this site in chow-fed apo E-/- mice progress from fatty streaks through stages that include atheroma with large necrotic areas, fibro-fatty nodules containing chondrocyte-like cells and highly calcified, acellular plaques. The advanced lesions in the innominate arteries of the apo E-/- mice exhibit a reproducible frequency of intra-plaque hemorrhage that occurs primarily as a result of fissures through lateral fatty streaks that form adjacent to or on top of the established plaques. However, this plaque disruption is not equivalent to plaque rupture in human lesions where there is rupture of well formed fibrous caps. The plaque disruption in the lesions of the chow-fed apo E-/- mice also do not lead to formation of occlusive thrombi, the predominant marker of plaque rupture in humans. Thus, although the lesions in the innominate arteries of hyperlipidemic mice progress to very advanced stages of the disease, they are not, in our opinion a model in which to study the mechanisms of plaque rupture in humans. The advanced lesions in the innominate arteries of the apo E-/- mice may however be adequate models for studying vascular fibrosis and calcification.

摘要

无名动脉是高脂血症小鼠动脉粥样硬化病变形成的好发部位。在喂食普通饲料的载脂蛋白E基因敲除(apo E-/-)小鼠中,该部位的病变从脂肪条纹开始发展,历经多个阶段,包括伴有大面积坏死区域的动脉粥样瘤、含有软骨样细胞的纤维脂肪结节以及高度钙化的无细胞斑块。apo E-/-小鼠无名动脉中的晚期病变呈现出可重复的斑块内出血频率,这种出血主要是由于在已形成斑块相邻或上方形成的横向脂肪条纹出现裂隙所致。然而,这种斑块破裂与人类病变中的斑块破裂并不等同,人类病变中的斑块破裂是指形成良好的纤维帽发生破裂。喂食普通饲料的apo E-/-小鼠病变中的斑块破裂也不会导致闭塞性血栓形成,而闭塞性血栓形成是人类斑块破裂的主要标志。因此,尽管高脂血症小鼠无名动脉中的病变会发展到疾病的非常晚期阶段,但我们认为它们并非研究人类斑块破裂机制的合适模型。不过,apo E-/-小鼠无名动脉中的晚期病变可能是研究血管纤维化和钙化的合适模型。

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