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中国人群早发性帕金森病:99mTc-TRODAT-1单光子发射计算机断层扫描、帕金基因分析及临床研究

Early-onset Parkinson's disease in a Chinese population: 99mTc-TRODAT-1 SPECT, Parkin gene analysis and clinical study.

作者信息

Shyu Woei-Cherng, Lin Shinn-Zong, Chiang Ming-Fu, Pang Cheng-Yoong, Chen Shin-Yuan, Hsin Yue-Loong, Thajeb Peterus, Lee Yih-Jing, Li Hung

机构信息

Neuro-Medical Scientific Center, Tzu-Chi Buddhist General Hospital, Tzu-Chi University, Hualien, Taiwan.

出版信息

Parkinsonism Relat Disord. 2005 May;11(3):173-80. doi: 10.1016/j.parkreldis.2004.12.004.

DOI:10.1016/j.parkreldis.2004.12.004
PMID:15823482
Abstract

Early Onset Parkinson's Disease (EOPD) is characterized by selective degeneration of nigrostriatal dopaminergic neurons and a marked response to levodopa. However, at present, few methods are available as diagnostic tools for EOPD except for 18F-DOPA PET. In addition, little is known about the correlation between clinical severity, neuroimaging grading and genetic susceptibility. In the present study, 99mTc-TRODAT-1 SPECT and brain MRI were used to identify 30 cases of non-familial EOPD from a Chinese cohort of 230. All 30 PD patients had an age of onset of less than 55 years (mean age at onset, 41.5+/-9.3 years). Each of the 30 EOPD cases was sub-classified into one of five stages based on the 99mTc-TRODAT-1 SPECT findings. In the early stages of PD (stages 1 and 2), a lower uptake of 99mTc-TRODAT-1 in the putamen was found, while uptake in the caudate nucleus was normal. In the latter stages (stages 3, 4, 5), 24 patients revealed a diffuse and uniform loss of 99mTc-TRODAT-1 uptake in the putamen and the caudate nucleus. Further, in conventional genetic studies of the 30 patients, six novel mutations were found in the Parkin gene, and these included five heterozygous point mutations (C441R, Q311H, V258M, C212G, and S193I) and one homozygous deletion (exon 10-12). Known polymorphisms (Ser167Asn, Val380Leu) were also found in a number of patients. However, gene dosage analysis did not reveal any compound heterozygous mutations in these 30 patients using quantitative duplex PCR. This is the first study to examine EOPD patients of Chinese ethnic background (not exhibiting a definite familial trait), to offer a complete genetic analysis of the Parkin gene, and to correlate clinical stages of the disease with dopamine re-uptake.

摘要

早发性帕金森病(EOPD)的特征是黑质纹状体多巴胺能神经元选择性退化以及对左旋多巴有显著反应。然而,目前除了18F - DOPA PET外,几乎没有可用的方法作为EOPD的诊断工具。此外,关于临床严重程度、神经影像学分级和遗传易感性之间的相关性知之甚少。在本研究中,使用99mTc - TRODAT - 1单光子发射计算机断层扫描(SPECT)和脑部磁共振成像(MRI)从230例中国人队列中识别出30例非家族性EOPD。所有30例帕金森病患者的发病年龄均小于55岁(平均发病年龄为41.5±9.3岁)。根据99mTc - TRODAT - 1 SPECT检查结果,30例EOPD病例中的每一例都被分为五个阶段之一。在帕金森病的早期阶段(1期和2期),发现壳核中99mTc - TRODAT - 1摄取较低,而尾状核摄取正常。在后期阶段(3期、4期、5期),24例患者显示壳核和尾状核中99mTc - TRODAT - 1摄取弥漫性且均匀丧失。此外,在对这30例患者的常规基因研究中,在帕金基因中发现了6个新突变,其中包括5个杂合点突变(C441R、Q311H、V258M、C212G和S193I)和1个纯合缺失(外显子10 - 12)。在一些患者中还发现了已知的多态性(Ser167Asn、Val380Leu)。然而,使用定量双链PCR的基因剂量分析未在这30例患者中发现任何复合杂合突变。这是第一项对具有中国种族背景(未表现出明确家族特征)的EOPD患者进行研究,对帕金基因进行完整基因分析,并将疾病临床阶段与多巴胺再摄取相关联的研究。

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