Department of Neurology, Barrow Neurological Institute, Phoenix, Arizona.
Departments of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota.
Semin Neurol. 2020 Feb;40(1):97-115. doi: 10.1055/s-0039-3402061. Epub 2020 Jan 20.
Autoimmune disorders affecting the vestibular end organs, vestibular pathways, vestibular nuclei, and vestibulocerebellum are often underrecognized as a cause of chronic dizziness and ataxia. Autoantibodies specific for cell-surface, synaptic, and intracellular neural antigens serve as biomarkers of these disorders. This article describes the epidemiology, clinical presentation, diagnostic considerations, imaging findings, treatment, and prognosis of autoimmune disorders, in which the vestibulocerebellar syndrome is the main or presenting clinical presentation. Antibodies specific for intracellular antigenic targets described in the article are PCA-1 (Purkinje cell cytoplasmic antibody type 1, also known as anti-Yo), ANNA-1 (antinuclear neuronal antibody type 1, also known as anti-Hu), ANNA-2 (antinuclear neuronal antibody type 2, also known as anti-Ri), Ma1/2 (anti-Kelch-like 11/12 antibody), Kelch-like 11, amphiphysin, CV2 (collapsin response 2, also known as collapsin response mediator protein-5 [CRMP5]), VGCC (voltage-gated calcium channel), GAD65 (glutamic acid decarboxylase 65-kDa isoform), AP3B2 (adaptor protein 3B2, also known as anti-Nb), MAP1B (microtubule-associated protein 1B antibody, also known as anti-PCA-2), and neurochondrin antibodies. Antibodies targeting cell-surface or synaptic antigenic targets described in the article include DNER (delta/notchlike epidermal growth factor related receptor; antigen to anti-Tr), CASPR2 (contactin-associated proteinlike 2), septin-5, Homer-3, and mGluR1 (metabotropic glutamate receptor 1). The vestibulocerebellar presentation is largely indistinguishable among these conditions and is characterized by subacute onset of cerebellar symptoms over weeks to months. The diagnosis of autoimmune vestibulocerebellar syndromes is based on a combination of clinical and serological features, with a limited role for neuroimaging. Subtle eye movement abnormalities can be an early feature in many of these disorders, and therefore a meticulous vestibulo-ocular examination is essential for early and correct identification. Cancer occurrence and its type are variable and depend on the autoantibody detected and other cancer risk factors. Treatment comprises immunotherapy and cancer-directed therapy. Acute immunotherapies such as intravenous immunoglobulin, plasma exchange, and steroids are used in the initial phase, and the use of long-term immunosuppression such as rituximab may be necessary in relapsing cases. Outcomes are better if immunotherapy is started early. The neurologic prognosis depends on multiple factors.
影响前庭终器、前庭通路、前庭核和前庭小脑的自身免疫性疾病常被低估为慢性头晕和共济失调的原因。针对细胞表面、突触和细胞内神经抗原的自身抗体可作为这些疾病的生物标志物。本文描述了自身免疫性疾病的流行病学、临床表现、诊断注意事项、影像学表现、治疗和预后,其中前庭小脑综合征是主要或表现性临床特征。本文描述的针对细胞内抗原靶标的抗体包括 PCA-1(浦肯野细胞细胞质抗体 1,也称为抗 Yo)、ANNA-1(抗核神经元抗体 1,也称为抗 Hu)、ANNA-2(抗核神经元抗体 2,也称为抗 Ri)、Ma1/2(抗 Kelch-like 11/12 抗体)、Kelch-like 11、 amphiphysin、CV2( collapsin response 2,也称为 collapsin response mediator protein-5 [CRMP5])、VGCC(电压门控钙通道)、GAD65(谷氨酸脱羧酶 65-kDa 同工型)、AP3B2(衔接蛋白 3B2,也称为抗 Nb)、MAP1B(微管相关蛋白 1B 抗体,也称为抗 PCA-2)和神经软骨素抗体。本文描述的针对细胞表面或突触抗原靶标的抗体包括 DNER(delta/notch-like epidermal growth factor related receptor;抗原至抗-Tr)、CASPR2(contactin-associated proteinlike 2)、septin-5、 Homer-3 和 mGluR1(代谢型谷氨酸受体 1)。这些情况下的前庭小脑表现基本相同,其特征是小脑症状在数周到数月内亚急性发作。自身免疫性前庭小脑综合征的诊断基于临床和血清学特征的结合,神经影像学的作用有限。许多此类疾病的早期特征是微妙的眼动异常,因此,细致的前庭眼动检查对于早期和正确的识别至关重要。癌症的发生及其类型是可变的,取决于检测到的自身抗体和其他癌症危险因素。治疗包括免疫疗法和癌症靶向治疗。在初始阶段使用急性免疫疗法,如静脉注射免疫球蛋白、血浆置换和类固醇,在复发病例中可能需要使用长期免疫抑制治疗,如利妥昔单抗。如果早期开始免疫治疗,预后会更好。神经预后取决于多种因素。
