Neuro-ophthalmology Unit, Hopital Neurologique et Neurochirurgical P Wertheimer, Hospices Civils de Lyon, Lyon, France.
ENT, Cervico-Facial Surgery and Audiophonology, Hôpital Edouard Herriot, Hospices Civils de Lyon, F-69003, Lyon, France.
Cerebellum. 2021 Oct;20(5):687-700. doi: 10.1007/s12311-020-01192-w. Epub 2020 Oct 4.
The syndrome of cerebellar ataxia with neuropathy and bilateral vestibular areflexia (CANVAS) has emerged progressively during the last 30 years. It was first outlined by the neurootology/neurophysiology community in the vestibular areflexic patients, through the description of patients slowly developing late-onset cerebellar ataxia and bilateral vestibulopathy. The characteristic deficit of visuo-vestibulo-ocular reflex (VVOR) due to the impaired slow stabilizing eye movements was put forward and a specific disease subtending this syndrome was suggested. The association to a peripheral sensory axonal neuropathy was described later on, with neuropathological studies demonstrating that both sensory neuropathy and vestibular areflexia were diffuse ganglionopathy. Clinical and electrophysiological criteria of CANVAS were then proposed in 2016. Besides the classical triad, frequent chronic cough, signs of dysautonomia and neurogenic pains were frequently observed. From the beginning of published cohorts, sporadic as well as familial cases were reported, the last suggestive of an autosomal recessive mode of transmission. The genetic disorder was discovered in 2019, under the form of abnormal biallelic expansion in the replication factor C subunit 1 (RFC1) in a population of late-onset ataxia. This pathological expansion was found in 100% of the familial form and 92% of sporadic ones when the triad was complete. But using the genetic criteria, the phenotype of CANVAS seems to expand, for exemple including patients with isolated neuronopathy. We propose here to review the clinical, electrophysiological, anatomical, genetic aspect of CANVAS in light of the recent discovery of the genetic aetiology, and discuss differential diagnosis, neuropathology and physiopathology.
小脑性共济失调伴多发性神经病和双侧前庭反射消失(CANVAS)综合征在过去 30 年中逐渐出现。最初由神经耳科学/神经生理学界在前庭反射消失的患者中提出,通过描述患者逐渐出现迟发性小脑性共济失调和双侧前庭病。由于慢相眼动稳定功能受损导致视-前庭-眼反射(VVOR)的特征性缺陷被提出,并提出了这种综合征的特定疾病。后来描述了与周围感觉轴索性神经病的关联,神经病理学研究表明感觉神经病和前庭反射消失都是弥漫性神经节病。2016 年提出了 CANVAS 的临床和电生理标准。除了经典三联征外,还经常观察到慢性咳嗽、自主神经功能障碍和神经源性疼痛的体征。从已发表的队列开始,既报告了散发性病例,也报告了家族性病例,后者提示常染色体隐性遗传模式。遗传疾病是在 2019 年发现的,其形式为复制因子 C 亚基 1(RFC1)的异常双等位基因扩增,在迟发性共济失调人群中。当三联征完整时,这种病理性扩增在家族性形式中发现 100%,散发性形式中发现 92%。但是,根据遗传标准,CANVAS 的表型似乎在扩大,例如包括孤立性神经元病患者。我们在此回顾 CANVAS 的临床、电生理、解剖和遗传方面,结合最近发现的遗传病因,并讨论鉴别诊断、神经病理学和病理生理学。
