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体内实验模型能否反映人类脑小血管疾病?一项系统评价。

Do in vivo experimental models reflect human cerebral small vessel disease? A systematic review.

作者信息

Hainsworth Atticus H, Markus Hugh S

机构信息

Centre for Clinical Neuroscience, Division of Cardiac and Vascular Sciences, St George's University of London, London, UK.

出版信息

J Cereb Blood Flow Metab. 2008 Dec;28(12):1877-91. doi: 10.1038/jcbfm.2008.91. Epub 2008 Aug 13.

DOI:10.1038/jcbfm.2008.91
PMID:18698331
Abstract

Cerebral small vessel disease (SVD) is a major cause of stroke and dementia. Pathologically, three lesions are seen: small vessel arteriopathy, lacunar infarction, and diffuse white matter injury (leukoaraiosis). Appropriate experimental models would aid in understanding these pathologic states and also in preclinical testing of therapies. The objective was to perform a systematic review of animal models of SVD and determine whether these resemble four key clinicopathologic features: (1) small, discrete infarcts; (2) small vessel arteriopathy; (3) diffuse white matter damage; (4) cognitive impairment. Fifteen different models were included, under four categories: (1) embolic injuries (injected blood clot, photochemical, detergent-evoked); (2) hypoperfusion/ischaemic injury (bilateral common carotid occlusion/stenosis, striatal endothelin-1 injection, striatal mitotoxin 3-NPA); (3) hypertension-based injuries (surgical narrowing of the aorta, or genetic mutations, usually in the renin-angiotensin system); (4) blood vessel damage (injected proteases, endothelium-targeting viral infection, or genetic mutations affecting vessel walls). Chronic hypertensive models resembled most key features of SVD, and shared the major risk factors of hypertension and age with human SVD. The most-used model was the stroke-prone spontaneously hypertensive rat (SHR-SP). No model described all features of the human disease. The optimal choice of model depends on the aspect of pathophysiology being studied.

摘要

脑小血管病(SVD)是中风和痴呆的主要病因。在病理上,可观察到三种病变:小血管动脉病变、腔隙性梗死和弥漫性白质损伤(脑白质疏松症)。合适的实验模型将有助于理解这些病理状态,也有助于疗法的临床前测试。目的是对SVD的动物模型进行系统综述,并确定这些模型是否类似于四个关键的临床病理特征:(1)小的、离散的梗死灶;(2)小血管动脉病变;(3)弥漫性白质损伤;(4)认知障碍。纳入了15种不同的模型,分为四类:(1)栓塞性损伤(注射血凝块、光化学、洗涤剂诱发);(2)低灌注/缺血性损伤(双侧颈总动脉闭塞/狭窄、纹状体内皮素-1注射、纹状体线粒体毒素3-NPA);(3)基于高血压的损伤(主动脉手术缩窄,或基因突变,通常在肾素-血管紧张素系统);(4)血管损伤(注射蛋白酶、靶向内皮的病毒感染,或影响血管壁的基因突变)。慢性高血压模型类似于SVD的大多数关键特征,并且与人类SVD共享高血压和年龄这两个主要风险因素。最常用的模型是易中风自发性高血压大鼠(SHR-SP)。没有模型描述了人类疾病的所有特征。模型的最佳选择取决于所研究的病理生理学方面。

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