Elijah Lackey, Ariel Lefland, Christopher Eckstein
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引用次数: 0
摘要
一名 51 岁的男性患者患有已知的勒伯遗传性视神经病变(LHON),下肢无力和麻木症状不断加重。在两年前的一次脊髓病发后,他一直靠助行器行走,但两周后就只能坐轮椅了。他还出现了T4皮层以下对轻触、针刺和振动的感觉障碍。他的颈椎和胸椎核磁共振成像显示,从C2延伸到T12的T2高强度病变没有增强。两年前,他在就诊时被发现患有纵向广泛性脊髓病,这归因于他的 LHON。基因检测显示,他的基因从 3635 个鸟嘌呤变为腺嘌呤。当时的核磁共振成像显示,C1-T10病变累及中央和后部脊髓,但与新病变不同的是,没有累及腹侧和外侧角。鉴于他的病症与之前的病症相似,且对其他病因的评估结果为阴性,因此认为他是继发于 Leber's Plus 的复发性脊髓病。据我们所知,专门因 Leber's Plus 的 G3635A 突变而导致复发性脊髓病的病例以前从未报道过。
Leber's Hereditary Optic Neuropathy Plus Causing Recurrent Myelopathy due to an MT-DN1 Mutation at G3635A.
A 51-year-old man with known Leber's hereditary optic neuropathy (LHON) presented with worsening lower extremity weakness and numbness. Following an episode of myelopathy two years before, he had been ambulating with a walker but over two weeks became wheelchair bound. He also developed a sensory level below the T4 dermatome to light touch, pinprick, and vibration. MRI of his cervical and thoracic spine showed a nonenhancing T2 hyperintense lesion extending from C2 to T12. At his presentation two years earlier, he was found to have a longitudinally extensive myelopathy attributed to his LHON. Genetic testing revealed a 3635 guanine to adenine mutation. MRI at that presentation demonstrated a C1-T10 lesion involving the central and posterior cord but, unlike the new lesion, did not involve the ventral and lateral horns. Given the similarity to his prior presentation and a negative evaluation for alternative etiologies, he was thought to have recurrent myelopathy secondary to Leber's Plus. To our knowledge, recurrent myelopathy due specifically to the G3635A mutation in Leber's Plus has not been reported previously.
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