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小纤维疼痛性神经病变的病理学与功能诊断

Pathology and functional diagnosis of small-fiber painful neuropathy.

作者信息

Hsieh Sung-Tsang

机构信息

Department of Neurology, National Taiwan University Hospital and Department of Anatomy and Cell Biology, National Taiwan University College of Medicine, Taipei, Taiwan.

出版信息

Acta Neurol Taiwan. 2010 Jun;19(2):82-9.

PMID:20714957
Abstract

Small-fiber sensory neuropathy with neuropathic pain had been a diagnostic challenge for neurologists. We and several groups have developed skin biopsy with quantitation of intraepidermal nerve fiber (IENF) density as a diagnostic approach. In the skin with small-fiber sensory neuropathy, there are pathological hallmarks: reduced IENF density with degeneration of subepidermal nerve plexuses and dermal nerves. Skin denervation is a major presentation of diabetic neuropathy and inflammatory neuropathies including Guillain-Barr syndrome and chronic inflammatory demyelinating polyneuropathy. The skin biopsy approach also provides an opportunity to examine dermal vasculature and inflammatory vasculopathy is demonstrated in vasculitic neuropathy, systemic lupus erythematosus, and eosinophilia-associated neuropathy. In addition to neuropahtologic evidence, the functional consequences of cutaneous nerve degeneration can be assessed with quantitative sensory testing (QST), contact heat evoked potential (CHEP), and functional magnetic resonance imaging (fMRI). One major etiology of small-fiber sensory neuropathy is familial amyloid polyneuropathy caused by mutations of transthyretin (TTR). We recently conducted studies on a large cohort of unique TTR mutation on Ala97Ser in Taiwan. These patients had significant skin denervation in addition to motor and autonomic neuropathy. Taken together, the skin biopsy with quantitation of IENF density provides diagnostic utility for small-fiber sensory neuropathy and the combination of psychophysical, physiological, and neuroimaging examinations offer comprehensive assessments for patients with neuropathic pain due o cutaneous nerve degeneration.

摘要

伴有神经病理性疼痛的小纤维感觉神经病一直是神经科医生面临的诊断挑战。我们和其他几个团队已经开发出通过定量表皮内神经纤维(IENF)密度的皮肤活检作为一种诊断方法。在患有小纤维感觉神经病的皮肤中,存在病理特征:IENF密度降低,同时表皮下神经丛和真皮神经发生退化。皮肤去神经支配是糖尿病性神经病以及包括格林-巴利综合征和慢性炎症性脱髓鞘性多发性神经病在内的炎性神经病的主要表现。皮肤活检方法还提供了检查真皮血管系统的机会,并且在血管炎性神经病(如系统性红斑狼疮和嗜酸性粒细胞增多相关神经病)中可证实存在炎性血管病变。除了神经病理学证据外,还可以通过定量感觉测试(QST)、接触热诱发电位(CHEP)和功能磁共振成像(fMRI)来评估皮肤神经变性的功能后果。小纤维感觉神经病的一个主要病因是由转甲状腺素蛋白(TTR)突变引起的家族性淀粉样多神经病。我们最近对台湾一大群具有独特的Ala97Ser TTR突变的患者进行了研究。这些患者除了存在运动和自主神经病变外,还存在明显的皮肤去神经支配。综上所述,定量IENF密度的皮肤活检为小纤维感觉神经病提供了诊断效用,而心理物理学、生理学和神经影像学检查的结合为因皮肤神经变性导致神经病理性疼痛的患者提供了全面评估。

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