Acute unilateral vestibulopathy/vestibular neuritis: Diagnostic criteria.

IF 2.9 3区 医学 Q2 NEUROSCIENCES
Michael Strupp, Alexandre Bisdorff, Joseph Furman, Jeremy Hornibrook, Klaus Jahn, Raphael Maire, David Newman-Toker, Måns Magnusson
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引用次数: 28

Abstract

This paper describes the diagnostic criteria for Acute Unilateral Vestibulopathy (AUVP), a synonym for vestibular neuritis, as defined by the Committee for the Classification of Vestibular Disorders of the Bárány Society. AUVP manifests as an acute vestibular syndrome due to an acute unilateral loss of peripheral vestibular function without evidence for acute central or acute audiological symptoms or signs. This implies that the diagnosis of AUVP is based on the patient history, bedside examination, and, if necessary, laboratory evaluation. The leading symptom is an acute or rarely subacute onset of spinning or non-spinning vertigo with unsteadiness, nausea/vomiting and/or oscillopsia. A leading clinical sign is a spontaneous peripheral vestibular nystagmus, which is direction-fixed and enhanced by removal of visual fixation with a trajectory appropriate to the semicircular canal afferents involved (generally horizontal-torsional). The diagnostic criteria were classified by the committee for four categories: 1. "Acute Unilateral Vestibulopathy", 2. "Acute Unilateral Vestibulopathy in Evolution", 3. "Probable Acute Unilateral Vestibulopathy" and 4. "History of Acute Unilateral Vestibulopathy". The specific diagnostic criteria for these are as follows:"Acute Unilateral Vestibulopathy": A) Acute or subacute onset of sustained spinning or non-spinning vertigo (i.e., an acute vestibular syndrome) of moderate to severe intensity with symptoms lasting for at least 24 hours. B) Spontaneous peripheral vestibular nystagmus with a trajectory appropriate to the semicircular canal afferents involved, generally horizontal-torsional, direction-fixed, and enhanced by removal of visual fixation. C) Unambiguous evidence of reduced VOR function on the side opposite the direction of the fast phase of the spontaneous nystagmus. D) No evidence for acute central neurological, otological or audiological symptoms. E) No acute central neurological signs, namely no central ocular motor or central vestibular signs, in particular no pronounced skew deviation, no gaze-evoked nystagmus, and no acute audiologic or otological signs. F) Not better accounted for by another disease or disorder."Acute Unilateral Vestibulopathy in Evolution": A) Acute or subacute onset of sustained spinning or non-spinning vertigo with continuous symptoms for more than 3 hours, but not yet lasting for at least 24 h hours, when patient is seen; B) - F) as above. This category is useful for diagnostic reasons to differentiate from acute central vestibular syndromes, to initiate specific treatments, and for research to include patients in clinical studies."Probable Acute Unilateral Vestibulopathy": Identical to AUVP except that the unilateral VOR deficit is not clearly observed or documented."History of acute unilateral vestibulopathy": A) History of acute or subacute onset of vertigo lasting at least 24 hours and slowly decreasing in intensity. B) No history of simultaneous acute audiological or central neurological symptoms. C) Unambiguous evidence of unilaterally reduced VOR function. D) No history of simultaneous acute central neurological signs, namely no central ocular motor or central vestibular signs and no acute audiological or otological signs. E) Not better accounted for by another disease or disorder. This category allows a diagnosis in patients presenting with a unilateral peripheral vestibular deficit and a history of an acute vestibular syndrome who are examined well after the acute phase.It is important to note that there is no definite test for AUVP. Therefore, its diagnosis requires the exclusion of central lesions as well as a variety of other peripheral vestibular disorders. Finally, this consensus paper will discuss other aspects of AUVP such as etiology, pathophysiology and laboratory examinations if they are directly relevant to the classification criteria.

急性单侧前庭病变/前庭神经炎:诊断标准。
本文描述了急性单侧前庭病变(AUVP)的诊断标准,这是前庭神经炎的同义词,由Bárány社会前庭疾病分类委员会定义。AUVP表现为急性单侧外周前庭功能丧失引起的急性前庭综合征,无急性中枢或急性听力学症状或体征的证据。这意味着AUVP的诊断是基于患者病史、床边检查和必要时的实验室评估。主要症状是急性或罕见亚急性发作的旋转或非旋转性眩晕,伴有不稳定,恶心/呕吐和/或震颤。一个主要的临床症状是自发性外周前庭眼球震颤,其方向固定,并通过去除视觉固定而增强,其轨迹与所涉及的半规管传入事件(通常为水平扭转)相适应。诊断标准被委员会分为四类:1.诊断标准;《急性单侧前庭病变》;“进化中的急性单侧前庭病变”,第3期。“可能的急性单侧前庭病变”和4。“急性单侧前庭病变史”。具体诊断标准如下:“急性单侧前庭病变”:A)急性或亚急性发作持续性纺纱或非纺纱性眩晕(即急性前庭综合征),强度中等至重度,症状持续至少24小时。B)自发性外周前庭眼球震颤,其运动轨迹与受损伤的半规管传入活动相适应,通常为水平扭转,方向固定,移除视固定物后增强。C)明确的证据表明自发性眼球震颤快速相方向相反侧的VOR功能减少。D)无急性中枢神经、耳科或听力学症状的证据。E)无急性中枢神经体征,即无中枢眼运动或中枢前庭体征,特别是无明显的斜斜,无凝视诱发的眼球震颤,无急性听力学或耳力学体征。F)不能更好地解释另一种疾病或紊乱。“进化中的急性单侧前庭病变”:A)急性或亚急性发作的持续性纺纱或非纺纱性眩晕,持续症状超过3小时,但在就诊时尚未持续至少24小时;B) - F)如上所述。这一类别对于诊断原因与急性中枢性前庭综合征区分、启动特定治疗以及将患者纳入临床研究是有用的。“可能的急性单侧前庭病变”:与AUVP相同,但单侧VOR缺失未被清楚观察或记录。“急性单侧前庭病变史”:A)急性或亚急性眩晕发作史,持续至少24小时,强度缓慢下降。B)无同时急性听力学或中枢神经症状史。C)单侧VOR功能降低的明确证据。D)无同时出现急性中枢神经体征的病史,即无中枢眼运动或中枢前庭体征,无急性听力学或耳科学体征。E)不能更好地解释另一种疾病或失调。这一分类允许在出现单侧前庭外周缺损和有急性前庭综合征病史的患者在急性期后检查良好时进行诊断。值得注意的是,对于AUVP没有明确的测试方法。因此,其诊断需要排除中枢病变以及各种其他周围前庭疾病。最后,本文将讨论AUVP的其他方面,如病因、病理生理学和实验室检查,如果它们与分类标准直接相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
5.00
自引率
4.30%
发文量
66
审稿时长
>12 weeks
期刊介绍: Journal of Vestibular Research is a peer-reviewed journal that publishes experimental and observational studies, review papers, and theoretical papers based on current knowledge of the vestibular system. Subjects of the studies can include experimental animals, normal humans, and humans with vestibular or other related disorders. Study topics can include the following: Anatomy of the vestibular system, including vestibulo-ocular, vestibulo-spinal, and vestibulo-autonomic pathways Balance disorders Neurochemistry and neuropharmacology of balance, both at the systems and single neuron level Neurophysiology of balance, including the vestibular, ocular motor, autonomic, and postural control systems Psychophysics of spatial orientation Space and motion sickness Vestibular rehabilitation Vestibular-related human performance in various environments
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