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肿瘤神经抗体对于诊断副肿瘤性神经系统综合征至关重要。

Onconeural antibodies are essential to diagnose paraneoplastic neurological syndromes.

作者信息

Honnorat J

机构信息

Hôpital Pierre Wertheimer, Hospices Civils de Lyon and INSERM U433 and Institut Fédératif des Neurosciences, Lyon, France.

出版信息

Acta Neurol Scand Suppl. 2006;183:64-8. doi: 10.1111/j.1600-0404.2006.00620.x.

Abstract

Paraneoplastic neurological syndromes (PNS) can be defined as remote effects of cancer that are not caused by the tumor and its metastasis or by infection, ischemia or metabolic disruptions. In most patients, the neurological disorder develops before the cancer becomes clinically overt and the patient is referred to the neurologist who has the charge of identifying a neurological disorder as paraneoplastic. They are usually severely disabling. PNS are rare and are seen in less than 1% of patients with cancer. PNS depend on an autoimmune process triggered by cancer and directed to antigens common to both the cancer and the nervous system designated as onconeural antigens. Because of their high specificity (>90%), the best way to diagnose neurological disorders as paraneoplastic is to identify one of the well-characterized onconeural antibodies in the patient's serum. In addition, as these antibodies are associated with a restricted range of cancer, they permit orientating the search of the underlying tumor at a stage where it is frequently not clinically overt. This is a critical point, as today the best way to stabilize PNS is probably to treat the cancer as soon as possible. Unfortunately, about one-third of the patients do not have detectable antibodies and 5-10% have an atypical antibody that is not well characterized.

摘要

副肿瘤性神经系统综合征(PNS)可定义为癌症的远隔效应,并非由肿瘤及其转移、感染、缺血或代谢紊乱所致。在大多数患者中,神经系统疾病在癌症出现临床症状之前就已发生,患者会被转诊至负责将神经系统疾病诊断为副肿瘤性疾病的神经科医生处。这些疾病通常会导致严重的功能障碍。PNS较为罕见,在不到1%的癌症患者中出现。PNS依赖于由癌症触发并针对癌症和神经系统共有的抗原(即肿瘤神经抗原)的自身免疫过程。由于其高特异性(>90%),将神经系统疾病诊断为副肿瘤性疾病的最佳方法是在患者血清中识别出一种特征明确的肿瘤神经抗体。此外,由于这些抗体与特定范围的癌症相关,它们有助于在肿瘤通常尚未出现临床症状的阶段确定潜在肿瘤的搜索方向。这是一个关键点,因为如今稳定PNS的最佳方法可能是尽快治疗癌症。不幸的是,约三分之一的患者检测不到抗体,5% - 10%的患者有一种特征不明确的非典型抗体。

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