六个携带MELAS tRNA(Leu)A2343G点突变家系的神经放射学特征:对发病机制的启示
Neuroradiological features of six kindreds with MELAS tRNA(Leu) A2343G point mutation: implications for pathogenesis.
作者信息
Sue C M, Crimmins D S, Soo Y S, Pamphlett R, Presgrave C M, Kotsimbos N, Jean-Francois M J, Byrne E, Morris J G
机构信息
Department of Neurology, University of Sydney and Westmead Hospital, Australia.
出版信息
J Neurol Neurosurg Psychiatry. 1998 Aug;65(2):233-40. doi: 10.1136/jnnp.65.2.233.
OBJECTIVE
To determine the neuroradiological abnormalities associated with subjects carrying the mitochondrial myopathy, encephalopathy, lactic acidosis, and strokelike episodes (MELAS) tRNA(Leu)(UUR) A3243G point mutation
METHODS
Mitochondrial genetic analysis was performed on 24 subjects from six kindreds with the MELAS tRNA(Leu)(UUR) A3243G point mutation. Cerebral CT and MRI were performed on 24 patients and 15 patients respectively. Previous neuroradiological investigations including cerebral CT from four deceased members of the families were also reviewed. Histological examination of postmortem specimens of two patients within the kindreds was performed.
RESULTS
The commonest radiological finding was basal ganglia calcification. Other abnormalities included focal lesions and cerebellar and cerebral atrophy. Basal ganglia calcification was progressive, symmetric, and asymptomatic. Histologically, basal ganglia calcification in one patient was found to be in the pericapillary regions of the globus pallidus, with no neuronal involvement. Focal lesions most commonly involved the grey matter of the parietal and occipital lobes and cerebellum. Histopathological examination suggested that these were due to cellular rather than vascular dysfunction. Enlargement of the fourth ventricle was the first sign of cerebellar atrophy. Cerebral and cerebellar atrophy were only present with severe disease.
CONCLUSIONS
These radiological findings, when considered in the context of the clinical and pathological findings, seem to reflect two major disease processes: an intermittent abrupt loss of function associated with cell injury from which there is at least partial recovery and a slowly progressive degenerative process causing basal ganglia calcification, and cerebral and cerebellar atrophy. The clinical and radiological features resulting from these processes are distinctive and provide insight into the consequences of mitochondrial dysfunction on the brain.
目的
确定与携带线粒体肌病、脑病、乳酸酸中毒和卒中样发作(MELAS)tRNA(Leu)(UUR) A3243G点突变的受试者相关的神经放射学异常
方法
对来自六个携带MELAS tRNA(Leu)(UUR) A3243G点突变家系的24名受试者进行线粒体基因分析。分别对24例患者和15例患者进行了脑部CT和MRI检查。还回顾了包括来自四个家族已故成员的脑部CT在内的既往神经放射学检查。对家系中两名患者的尸检标本进行了组织学检查。
结果
最常见的放射学表现是基底节钙化。其他异常包括局灶性病变以及小脑和脑萎缩。基底节钙化呈进行性、对称性且无症状。组织学上,一名患者的基底节钙化位于苍白球的毛细血管周围区域,无神经元受累。局灶性病变最常累及顶叶和枕叶以及小脑的灰质。组织病理学检查表明,这些是由于细胞功能障碍而非血管功能障碍所致。第四脑室扩大是小脑萎缩的首个征象。脑和小脑萎缩仅在病情严重时出现。
结论
结合临床和病理结果来看,这些放射学表现似乎反映了两个主要的疾病过程:与细胞损伤相关的间歇性突然功能丧失,至少有部分恢复;以及导致基底节钙化、脑和小脑萎缩的缓慢进行性退行性过程。这些过程导致的临床和放射学特征具有独特性,有助于深入了解线粒体功能障碍对大脑的影响。
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