Department of Molecular Neuroscience, UCL Institute of Neurology, London, United Kingdom.
Mov Disord. 2010 Sep 15;25(12):1791-800. doi: 10.1002/mds.23221.
Seven autosomal recessive genes associated with juvenile and young-onset Levodopa-responsive parkinsonism have been identified. Mutations in PRKN, DJ-1, and PINK1 are associated with a rather pure parkinsonian phenotype, and have a more benign course with sustained treatment response and absence of dementia. On the other hand, Kufor-Rakeb syndrome has additional signs, which distinguish it clearly from Parkinson's disease including supranuclear vertical gaze palsy, myoclonic jerks, pyramidal signs, and cognitive impairment. Neurodegeneration with brain iron accumulation type I (Hallervorden-Spatz syndrome) due to mutations in PANK2 gene may share similar features with Kufor-Rakeb syndrome. Mutations in three other genes, PLA2G6 (PARK14), FBXO7 (PARK15), and Spatacsin (SPG11) also produce clinical similar phenotypes in that they presented with rapidly progressive parkinsonism, initially responsive to Levodopa treatment but later, developed additional features including cognitive decline and loss of Levodopa responsiveness. Here, using homozygosity mapping and sequence analysis in families with complex parkinsonisms, we identified genetic defects in the ATP13A2 (1 family), PLA2G6 (1 family) FBXO7 (2 families), and SPG11 (1 family). The genetic heterogeneity was surprising given their initially common clinical features. On careful review, we found the FBXO7 cases to have a phenotype more similar to PRKN gene associated parkinsonism. The ATP13A2 and PLA2G6 cases were more seriously disabled with additional swallowing problems, dystonic features, severe in some, and usually pyramidal involvement including pyramidal weakness. These data suggest that these four genes account for many cases of Levodopa responsive parkinsonism with pyramidal signs cases formerly categorized clinically as pallido-pyramidal syndrome.
已鉴定出与青少年和早发性左旋多巴反应性帕金森病相关的七个常染色体隐性基因。PRKN、DJ-1 和 PINK1 的突变与相当纯粹的帕金森病表型相关,并且具有更良性的病程,持续治疗反应和无痴呆。另一方面,Kufor-Rakeb 综合征具有其他体征,这使其明显区别于帕金森病,包括核上垂直凝视麻痹、肌阵挛性抽搐、锥体束征和认知障碍。由于 PANK2 基因突变导致的脑铁积累 I 型神经退行性变(Hallervorden-Spatz 综合征)可能与 Kufor-Rakeb 综合征具有相似的特征。另外三个基因 PLA2G6(PARK14)、FBXO7(PARK15)和 Spatacsin(SPG11)的突变也产生了临床相似的表型,即它们表现为快速进展性帕金森病,最初对左旋多巴治疗有反应,但后来出现了认知能力下降和失去左旋多巴反应性等其他特征。在这里,我们使用复杂帕金森病家系的纯合子作图和序列分析,鉴定了 ATP13A2(1 个家系)、PLA2G6(1 个家系)、FBXO7(2 个家系)和 SPG11(1 个家系)的遗传缺陷。鉴于它们最初的共同临床特征,遗传异质性令人惊讶。仔细审查后,我们发现 FBXO7 病例的表型更类似于与 PRKN 基因相关的帕金森病。ATP13A2 和 PLA2G6 病例的残疾程度更严重,伴有吞咽问题、张力障碍特征,在某些情况下更为严重,通常还伴有锥体束受累,包括锥体束无力。这些数据表明,这四个基因可解释许多伴有锥体束征的左旋多巴反应性帕金森病病例,这些病例以前临床上归类为苍白球-锥体束综合征。