Department of Neuropathology, Graduate School of Medical Sciences, Kyushu University, Fukuoka 812-8582, Japan.
Acta Neuropathol. 2011 Dec;122(6):775-81. doi: 10.1007/s00401-011-0916-x. Epub 2011 Nov 20.
We report an autopsy case of rare adult-onset spastic paraplegia type 2 (SPG2) with a novel missense mutation in exon 7 of the proteolipid protein 1 gene (PLP1). The patient was a 67-year-old man whose elder brother had died of a similar disease with onset in his 40s. Thirty-three years before death at the age of 35, he noticed difficulty in walking. He gradually became abasic over a period of 6 years. He also developed progressive dementia and eventually became bed-ridden by 28 years after onset. At autopsy, gross inspection revealed diffuse, moderate atrophy of the cerebrum with a dilated ventricular system and softening of the white matter throughout the central nervous system (CNS). Histopathologically, the CNS showed widespread myelin pallor in the white matter. By contrast, the gray matter and peripheral nerves were well preserved. Some white matter tracts, including the corticospinal tracts, were preferentially affected, and severe axonal degeneration was observed in these tracts. Genetic analysis revealed a novel mutation, p.Tyr263Cys, in exon 7 of PLP1. This case represents an adult-onset SPG2 patient with one of the oldest ages of onset reported to date. The late onset and long clinical course suggest that this novel mutation does not affect the maturation of oligodendrocytes, but is related to insufficient maintenance of myelin.
我们报告了一例罕见的成人起病的痉挛性截瘫 2 型(SPG2)的尸检病例,该病例在蛋白脂质蛋白 1 基因(PLP1)的外显子 7 中存在新的错义突变。患者是一名 67 岁男性,其哥哥在 40 多岁时死于类似疾病。在去世前 33 年,即 35 岁时,他注意到行走困难。他逐渐变得僵硬,持续了 6 年。他还出现进行性痴呆,最终在发病后 28 年卧床不起。尸检时,肉眼检查显示大脑弥漫性中度萎缩,脑室系统扩张,整个中枢神经系统(CNS)的白质软化。组织病理学检查显示,CNS 白质广泛出现髓磷脂苍白。相比之下,灰质和周围神经保存完好。一些白质束,包括皮质脊髓束,优先受到影响,并且在这些束中观察到严重的轴突变性。遗传分析显示 PLP1 外显子 7 中有一个新的突变,p.Tyr263Cys。该病例代表了一例成人起病的 SPG2 患者,其发病年龄是迄今为止报道的最年长的病例之一。发病晚和临床病程长提示该新突变不会影响少突胶质细胞的成熟,而是与髓磷脂的维持不足有关。
