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[隐源性脑梗死:从分类到概念]

[Cryptogenic cerebral infarction: from classification to concept].

作者信息

Timsit Serge, Breuilly Christophe

机构信息

CHU de la Cavale Blanche, Service de neurologie, F-29200 Brest, France.

出版信息

Presse Med. 2009 Dec;38(12):1832-42. doi: 10.1016/j.lpm.2009.02.012. Epub 2009 Apr 22.

Abstract

Since the foundations laid by Sacco and Mohr in 1989, from the Stroke data bank, cryptogenic infarctions have had a predominant place among the causes of ischemic strokes. In that study, they accounted for approximately 40% of the stroke causes. Cryptogenic infarctions are infarctions without a defined cause, despite a complete work-up; they differ from infarctions of undetermined causes, which may involve overlapping causes or an incomplete investigation. The size of this group will probably shrink as knowledge advances. Patent foramen ovale (PFO), with or without a septal aneurysm, is more frequent in patients with a cryptogenic infarction. Transesophageal echocardiography is the reference examination for screening for these abnormalities. A meta-analysis of several case-control studies showed a significant association between PFO and stroke in subjects younger than 55 years. For now, these septal abnormalities constitute a risk factor but not a cause. Complex aortic atheroma affecting area upstream of the left subclavian artery may be a source of cerebral embolisms in some conditions. The prevalence of this disease increases with age. It is identified most frequently in patients older than 60 years with a cryptogenic infarction. The thickness of the atheromatous plaque determines whether it is a risk factor or a cause. Recent stroke classifications do not consider carotid atheromatous lesions less than 50% to be a source of ischemic stroke. Nonetheless some studies identify moderate stenosis of the carotid artery more frequently in infarctions of unknown causes than in other categories. The increased risk of cerebral infarction when parents and homozygous twins have a history of stroke suggests that there may be genetic causes that have not yet been detected. An unknown genetic cause would thus be included in the infarctions of unknown causes. A recent study tested for Fabry disease in young patients with a cryptogenic infarction: 4.9% of the men and 2.4% of the women had a functional mutation of the alpha-galactosidase gene. These findings must be confirmed. Some studies suggest an association between cryptogenic infarction and hereditary thrombophilias. Nonetheless the risk attributable to these thrombophilic disorders is slight and the discovery may be only a coincidence. The work described above shows the importance of stratification in the identification of stroke causes: age older or younger than 55/60 years, type of interatrial abnormality (PFO and aneurysms of the interatrial septum), type of atheroma of the aortic arch (more or less than 4mm). They also show the difficulty involved in attributing cause to an identified abnormality: is carotid stenosis of less than 50% a marker of atherosclerosis or also a cause of stroke? To continue improving our understanding of the mechanisms of strokes, new investigational techniques are under evaluation. They include magnetic resonance imaging (MRI), computed tomographic angiography (CT), positron emission tomography (PET) of carotid plaque and of the aortic arch, transcranial Doppler, cardiac recording by telemetry, and even new biological assays.

摘要

自1989年萨科和莫尔奠定基础以来,在中风数据库中,隐源性梗死在缺血性中风病因中一直占据主要地位。在该研究中,它们约占中风病因的40%。隐源性梗死是指尽管进行了全面检查仍无明确病因的梗死;它们与病因未明的梗死不同,后者可能涉及多种重叠病因或检查不完整。随着知识的进步,这一群体的规模可能会缩小。伴有或不伴有房间隔瘤的卵圆孔未闭(PFO)在隐源性梗死患者中更为常见。经食管超声心动图是筛查这些异常的参考检查。对多项病例对照研究的荟萃分析表明,在55岁以下的受试者中,PFO与中风之间存在显著关联。目前,这些房间隔异常构成一个危险因素而非病因。在某些情况下,累及左锁骨下动脉上游区域的复杂性主动脉粥样硬化可能是脑栓塞的一个来源。这种疾病的患病率随年龄增长而增加。在60岁以上患有隐源性梗死的患者中最常发现。动脉粥样硬化斑块的厚度决定了它是一个危险因素还是病因。最近的中风分类不认为颈动脉粥样硬化病变小于50%是缺血性中风的一个来源。尽管如此,一些研究发现,在病因不明的梗死中,颈动脉中度狭窄比在其他类型中更常见。当父母和同卵双胞胎有中风病史时,脑梗死风险增加表明可能存在尚未被发现的遗传病因。因此,一种未知的遗传病因将被纳入病因不明的梗死中。最近一项针对年轻隐源性梗死患者的研究检测了法布里病:4.9%的男性和2.4%的女性有α-半乳糖苷酶基因的功能性突变。这些发现必须得到证实。一些研究表明隐源性梗死与遗传性血栓形成倾向之间存在关联。尽管如此,这些血栓形成性疾病所致的风险很小,这一发现可能只是巧合。上述研究表明了分层在确定中风病因中的重要性:年龄大于或小于55/60岁、房间隔异常类型(PFO和房间隔瘤)、主动脉弓粥样硬化类型(大于或小于4mm)。它们还表明将病因归因于已确定的异常存在困难:小于50%的颈动脉狭窄是动脉粥样硬化的一个标志还是也是中风的一个病因?为了继续增进我们对中风机制的理解,新的研究技术正在评估中。它们包括磁共振成像(MRI)、计算机断层血管造影(CT)、颈动脉斑块和主动脉弓的正电子发射断层扫描(PET)、经颅多普勒、通过遥测进行心脏记录,甚至新的生物学检测。

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