在法布里病、转甲状腺素蛋白相关家族性淀粉样变性和庞贝病中可通过因果关系进行治疗的遗传性神经病变。
Causally treatable, hereditary neuropathies in Fabry's disease, transthyretin-related familial amyloidosis, and Pompe's disease.
作者信息
Finsterer J, Wanschitz J, Quasthoff S, Iglseder S, Löscher W, Grisold W
机构信息
Krankenanstalt Rudolfstiftung, Vienna, Austria.
Department of Neurology, Medical University Innsbruck, Innsbruck, Austria.
出版信息
Acta Neurol Scand. 2017 Dec;136(6):558-569. doi: 10.1111/ane.12758. Epub 2017 Mar 12.
OBJECTIVES
Most acquired neuropathies are treatable, whereas genetic neuropathies respond to treatment in Fabry's disease (FD), transthyretin-related familial amyloidosis (TTR-FA), and Pompe's disease (PD). This review summarizes and discusses recent findings and future perspectives concerning etiology, pathophysiology, clinical presentation, diagnosis, treatment, and outcome of neuropathy in FD, TTR-FA, and PD.
METHODS
Literature review.
RESULTS
Neuropathy in FD concerns particularly small, unmyelinated, or myelinated sensory fibers (small fiber neuropathy [SFN]) and autonomic fibers, manifesting as acroparesthesias, Fabry's crises, or autonomous disturbances. FD neuropathy benefits from agalsidase alpha (0.2 mg/kg every second week intravenously) or from beta (1.0 mg/kg every second week intravenously). Neuropathy in TTR-FA is axonal and affects large and small sensory, motor, and autonomous fibers. Neuropathy in TTR-FA profits from liver transplantation and the TTR kinetic stabilizer tafamidis (20 mg/d). Neuropathy in PD particularly occurs in late-onset PD and manifests as mononeuropathy, polyneuropathy, or SFN. PD neuropathy presumably responds to alglucosidase-alpha (20 mg/kg every second week intravenously).
CONCLUSIONS
Neuropathy in FD, TTR-FA, and PD is predominantly a SFN and can be the dominant feature in FD and TTR-FA. SFN in FD, TTR-FA, and PD needs to be recognized and benefits from enzyme replacement treatment or TT-kinetic stabilizers.
目的
大多数获得性神经病变是可治疗的,而遗传性神经病变在法布里病(FD)、转甲状腺素蛋白相关家族性淀粉样变性(TTR-FA)和庞贝病(PD)中对治疗有反应。本综述总结并讨论了关于FD、TTR-FA和PD中神经病变的病因、病理生理学、临床表现、诊断、治疗及预后的最新研究结果和未来展望。
方法
文献综述。
结果
FD中的神经病变尤其涉及细小的无髓或有髓感觉纤维(小纤维神经病变[SFN])和自主神经纤维,表现为肢端感觉异常、法布里危象或自主神经功能障碍。FD神经病变可受益于α-半乳糖苷酶(每两周静脉注射0.2mg/kg)或β-半乳糖苷酶(每两周静脉注射1.0mg/kg)。TTR-FA中的神经病变是轴索性的,影响大小不等的感觉、运动和自主神经纤维。TTR-FA中的神经病变可从肝移植和TTR动力学稳定剂tafamidis(20mg/d)中获益。PD中的神经病变尤其发生在晚发型PD中,表现为单神经病变、多神经病变或SFN。PD神经病变可能对α-葡萄糖苷酶(每两周静脉注射20mg/kg)有反应。
结论
FD、TTR-FA和PD中的神经病变主要是SFN,并且可能是FD和TTR-FA中的主要特征。FD、TTR-FA和PD中的SFN需要被识别出来,并且可从酶替代治疗或TTR动力学稳定剂中获益。
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