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首页> 外文期刊>Clinical neurophysiology >Electrophysiological characterisation in hereditary spastic paraplegia type 5.
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Electrophysiological characterisation in hereditary spastic paraplegia type 5.

机译:5型遗传性痉挛性截瘫的电生理特征

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OBJECTIVE: To assess in SPG5 hereditary spastic paraparesis (HSP) the involvement of the central (CNS) and the peripheral (PNS) nervous system by a multimodal electrophysiological approach. METHODS: Four patients belonging to three HSP families, with a molecular diagnosis of SPG5, underwent electrophysiological evaluation including electromyography (EMG) and nerve conduction study (NCS), motor-evoked potentials (MEPs) by transcranial magnetic stimulation (TMS) and somatosensory evoked potentials (SEPs) at upper and lower limbs, visual (VEPs) and brainstem auditory evoked potentials (BAEPs). In one patient, electrophysiological evaluation was performed twice at the age of 12 and 31 years. RESULTS: EMG and NCS were normal. MEPs and SEPs were abnormal in all patients along the central pathway for upper and/or lower limbs. VEPs revealed a damage of visual pathway and BAEPs showed the involvement of auditory pathway within the brainstem. In the patient who underwent electrophysiological follow-up, MEP and SEP findings were unmodified, whereas VEPs showed no reproducible responses. CONCLUSIONS: We report an extensive electrophysiological evaluation of SPG5 and we confirm that the SPG5 phenotype may be broader than pure presentation. SIGNIFICANCE: Electrophysiological evaluation, showing diffuse CNS involvement with PNS sparing, could be very useful to address the molecular diagnosis and to follow-up a hypothetical treatment.
机译:目的:通过多模式电生理方法评估SPG5遗传性痉挛性轻瘫(HSP)对中枢(CNS)和末梢(PNS)神经系统的影响。方法:对四个属于HSP家族的4名患者进行分子诊断为SPG5,进行了电生理评估,包括肌电图(EMG)和神经传导研究(NCS),经颅磁刺激(TMS)诱发的运动诱发电位(MEP)和诱发体感上肢和下肢的电位(SEP),视觉(VEP)和脑干听觉诱发电位(BAEP)。在一名患者中,在12岁和31岁时进行了两次电生理评估。结果:EMG和NCS均正常。所有患者的上肢和/或下肢中央路径的MEP和SEP均异常。 VEPs显示视觉通路受损,BAEPs显示听觉通路参与脑干。在接受电生理随访的患者中,MEP和SEP的发现未改变,而VEPs则没有可再现的反应。结论:我们报告了SPG5的广泛电生理评估,并且我们确认SPG5的表型可能比纯表型更广泛。意义:电生理评估显示弥漫性的中枢神经系统受累于PNS保留,对解决分子诊断和随访假想治疗可能非常有用。

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