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下跳性眼球震颤:病变的特征与定位

Downbeat nystagmus: characteristics and localization of lesions.

作者信息

Yee R D

机构信息

Department of Ophthalmology, Indiana University, Indianapolis.

出版信息

Trans Am Ophthalmol Soc. 1989;87:984-1032.

Abstract

Clinical examinations and eye movement recordings of 91 consecutive patients with DBN were analyzed to describe the characteristics of DBN and to localize the lesions producing this abnormality. Horizontal and vertical eye movement recordings were made with EOG and/or magnetic search coil. The most frequent causes were infarction, cerebellar and spinocerebellar degeneration syndromes, MS and developmental anomalies affecting the pons and cerebellum. Toxicity from anticonvulsant drugs probably caused nystagmus in a few patients. Clinical examinations, excluding electronic eye movement recordings, were used to localize lesions. Localizations included the cerebellum in 88% of the patients. However, localizations to structures outside of the cerebellum were made in several patients. The effects of DBN of gaze position, convergence, blockage of fixation, and positioning of the head and body were observed. Almost all patients had DBN in some position of gaze while sitting and fixating a distant target. A few patients demonstrated DBN only with convergence, in the dark, or with positioning of the head and body. Horizontal gaze increased DBN in most patients. The nystagmus slow components usually had constant-velocity or increasing-velocity waveforms. The effects of vertical gaze on DBN were variable. In general, statistically significant differences in the frequencies of these effects among the various causes and localizations of lesions were not found. Horizontal eye movements were electronically recorded in DBN patients, in a group of normal subjects, and in a group of patients with isolated cerebellar atrophy who did not have DBN. The pattern of abnormal horizontal eye movements characteristic of damage to the midline structures of the cerebellum (impaired pursuit, impaired OKN, and inability to suppress VOR) was found in almost all DBN patients (99%), including patients with lesions localized to structures outside the cerebellum by clinical examination. DBN is usually produced by lesions in the cerebellum that also damage pathways that control horizontal tracking and visual-vestibulo-ocular interactions.

摘要

对91例连续性DBN患者进行了临床检查和眼动记录分析,以描述DBN的特征并确定产生这种异常的病变部位。采用EOG和/或磁性搜索线圈进行水平和垂直眼动记录。最常见的病因是梗死、小脑和脊髓小脑变性综合征、多发性硬化以及影响脑桥和小脑的发育异常。抗惊厥药物的毒性可能在少数患者中导致眼球震颤。临床检查(不包括电子眼动记录)用于确定病变部位。88%的患者病变部位在小脑。然而,有几名患者病变部位定位于小脑以外的结构。观察了DBN对注视位置、集合、注视阻断以及头部和身体位置的影响。几乎所有患者在坐位注视远处目标的某些注视位置时都有DBN。少数患者仅在集合、黑暗中或头部和身体位置改变时出现DBN。大多数患者水平注视时DBN增强。眼球震颤慢相成分通常具有等速或增速波形。垂直注视对DBN的影响各不相同。一般来说,在病变的各种病因和部位之间,这些影响的频率在统计学上没有显著差异。对DBN患者、一组正常受试者以及一组无DBN的孤立性小脑萎缩患者进行了水平眼动的电子记录。几乎所有DBN患者(99%)都发现了小脑中线结构损伤特有的异常水平眼动模式(追踪受损、视动性眼震受损以及无法抑制前庭眼反射),包括临床检查显示病变部位定位于小脑以外结构的患者。DBN通常由小脑病变引起,这些病变也会损害控制水平追踪和视-前庭-眼相互作用的通路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cf1a/1298566/3c6e98540079/taos00012-1023-a.jpg

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