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血管性痴呆和血管性认知障碍的实验模型:系统评价。

Experimental models of vascular dementia and vascular cognitive impairment: a systematic review.

机构信息

Clinical Neuroscience, Division of Clinical Sciences, St George's University of London, London, UK.

出版信息

J Neurochem. 2010 Nov;115(4):814-28. doi: 10.1111/j.1471-4159.2010.06958.x. Epub 2010 Oct 7.

Abstract

Vascular cognitive impairment (VCI) encompasses vascular dementia and is the second most common cause of dementing illness after Alzheimer's disease. The main causes of VCI are: cerebral small vessel disease; multi-infarct dementia; strategic infarct (i.e. located in a functionally-critical brain area); haemorrhage/microbleed; angiopathy (including cerebral amyloid angiopathy); severe hypoperfusion (e.g. cardiac arrhythmia); and hereditary vasculopathy (e.g. cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy, CADASIL). In this systematic analysis, we aimed to relate cognitive and neuropathological features of experimental models to clinical VCI. We extracted data from 107 studies covering 16 models. These included: brief global ischaemic insults (in rats, mice or gerbils); chronic global hypoperfusion (rats, mice, gerbils); chronic hypertension (in primates or stroke-prone, spontaneously-hypertensive rats); multiple ischaemic lesions because of intra-vascular emboli (in rodents, rabbits or primates); strategic ischaemic lesions (in rats or mini-pigs); generalised vasculopathies, because of mutant Notch3, hyperhomocysteinaemia, experimental diabetes mellitus or lack of cerebral vasodilator M(5) receptors (rats or mice). Most cognitive testing showed deficits in working and reference memory. The lesions observed were microinfarcts, diffuse white matter lesions, hippocampal neuronal death, focal ischaemic lesions and micro-haemorrhages. The most-used model was bilateral carotid artery occlusion in rats, leading to chronic hypoperfusion and white matter injury.

摘要

血管性认知障碍(VCI)包括血管性痴呆,是仅次于阿尔茨海默病的第二大痴呆病因。VCI 的主要病因包括:脑小血管病;多发性脑梗死性痴呆;局灶性梗死(即位于功能关键脑区);出血/微出血;血管病变(包括脑淀粉样血管病);严重低灌注(如心律失常);遗传性血管病(如伴有皮质下梗死和白质脑病的脑常染色体显性动脉病、CADASIL)。在这项系统分析中,我们旨在将实验模型的认知和神经病理学特征与临床 VCI 相关联。我们从涵盖 16 种模型的 107 项研究中提取数据。这些模型包括:短暂全脑缺血性损伤(在大鼠、小鼠或沙鼠中);慢性全脑低灌注(在大鼠、小鼠、沙鼠中);慢性高血压(在灵长类动物或易发生卒中、自发性高血压大鼠中);由于血管内栓塞导致的多次缺血性损伤(在啮齿动物、兔或灵长类动物中);局灶性缺血性损伤(在大鼠或小型猪中);由于突变型 Notch3、高同型半胱氨酸血症、实验性糖尿病或缺乏脑血管扩张剂 M5 受体引起的全身性血管病变(大鼠或小鼠)。大多数认知测试显示工作记忆和参考记忆缺陷。观察到的病变包括微梗死、弥漫性白质病变、海马神经元死亡、局灶性缺血性损伤和微出血。最常用的模型是大鼠双侧颈总动脉闭塞,导致慢性低灌注和白质损伤。

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