Cornejo-Olivas Mario R, Torres Luis, Mata Ignacio F, Mazzetti Pilar, Rivas Diana, Cosentino Carlos, Inca-Martinez Miguel, Cuba Juan M, Zabetian Cyrus P, Leverenz James B
Northern Pacific Global Health Research Fellows Training Consortium, Bethesda, MD, USA; Neurogenetics Research Center, Instituto Nacional de Ciencias Neurologicas, Lima, Peru.
Movement Disorders Unit, Instituto Nacional de Ciencias Neurologicas, Lima, Peru.
Parkinsonism Relat Disord. 2015 May;21(5):444-8. doi: 10.1016/j.parkreldis.2015.01.005. Epub 2015 Jan 15.
Mutations in PARK2 result in autosomal recessive young onset Parkinson's disease (YOPD). Although there have been a number of reports on the clinical characteristics of PARK2-related PD, there is limited information available on the associated neuropathologic changes.
We describe the clinical and pathological characteristics of a Peruvian family with YOPD. The proband and one unaffected sibling were screened for PARK2 dosage and point mutations. One affected sibling had detailed neuropathologic examination.
Instituto Nacional de Ciencias Neurologicas (INCN) in Lima, Peru.
The proband and two of her four siblings developed YOPD and both parents were unaffected. The clinical course has been characterized by akinetic-rigid parkinsonism predominantly affecting the lower limbs and dyskinesias. Analysis of PARK2 showed that the proband is compound heterozygous for a novel acceptor splice site mutation in intron 5 (IVS5-1G>A) and an exon 7 deletion. Neuropathologic assessment of an affected sibling revealed severe neuronal loss in the substantia nigra (SN) and loss of tyrosine hydroxylase immunopositive fibers in the striatum. No Lewy body pathology was observed using standard histology or immunohistochemistry for α-synuclein.
Consistent with most neuropathologic reports of patients with PARK2 mutations, we did not observe Lewy body inclusions, despite marked SN degeneration and severe dopaminergic denervation of the striatum. These data describe a novel splice site mutation and further extend the clinicopathological characterization of PARK2-associated PD.
PARK2基因的突变会导致常染色体隐性早发型帕金森病(YOPD)。尽管已有多篇关于PARK2相关帕金森病临床特征的报道,但关于相关神经病理变化的信息却很有限。
我们描述了一个患有YOPD的秘鲁家族的临床和病理特征。对先证者和一名未患病的同胞进行了PARK2剂量和点突变筛查。对一名患病同胞进行了详细的神经病理学检查。
秘鲁利马的国家神经科学研究所(INCN)。
先证者及其四个兄弟姐妹中的两个患上了YOPD,父母均未患病。临床病程的特征为主要影响下肢的运动不能-强直型帕金森综合征和运动障碍。对PARK2的分析表明,先证者为内含子5(IVS5-1G>A)中的一个新的受体剪接位点突变和外显子7缺失的复合杂合子。对一名患病同胞的神经病理学评估显示,黑质存在严重的神经元丢失,纹状体中酪氨酸羟化酶免疫阳性纤维减少。使用标准组织学或α-突触核蛋白免疫组织化学未观察到路易小体病理改变。
与大多数关于PARK2突变患者的神经病理学报告一致,尽管黑质明显变性且纹状体存在严重的多巴胺能去神经支配,但我们未观察到路易小体包涵体。这些数据描述了一种新的剪接位点突变,并进一步扩展了PARK2相关帕金森病的临床病理特征。