挪威早发性帕金森病患者的基因鉴定
Genetic Identification in Early Onset Parkinsonism among Norwegian Patients.
作者信息
Gustavsson Emil K, Trinh Joanne, McKenzie Marna, Bortnick Stephanie, Petersen Maria Skaalum, Farrer Matthew J, Aasly Jan O
机构信息
Center for Applied Neurogenetics Djavad Mowafaghian Center for Brain Health Department of Medical Genetics University of British Columbia Vancouver British Columbia Canada.
Department of Neuroscience Norwegian University of Science and Technology Trondheim Norway.
出版信息
Mov Disord Clin Pract. 2017 May 23;4(4):499-508. doi: 10.1002/mdc3.12501. eCollection 2017 Jul-Aug.
BACKGROUND
An initial diagnosis of Parkinson's disease (PD) is challenging, especially in patients who have early onset and atypical disease. A genetic etiology for parkinsonism, when established, ends that diagnostic odyssey and may inform prognosis and therapy. The objective of this study was to elucidate the genetic etiology of parkinsonism in patients with early onset disease (age at onset <45 years).
METHODS
Whole-exome sequencing, copy number variability, and short tandem repeat analyses were performed. The analyses were focused on genes previously implicated in parkinsonism and dystonia in patients with early onset parkinsonism. Genotype-phenotype correlations were assessed using regression models.
RESULTS
The patient cohort was characterized by early onset, slowly progressive parkinsonism with a mean age at onset of 39.2 ± 5.0 years (n = 108). By 10 years of disease duration, the mean Hoehn & Yahr stage was 2.6 ± 0.8, the mean Unified Parkinson's Disease Rating Scale, part III (motor part) score was 24.9 ± 12.1 (n = 83), and 30 patients were cognitively impaired at the last examination (Montreal Cognitive Assessment score ≤ 26). Ten patients with typical early onset PD harbored homozygous or compound heterozygous mutations phosphatase and tensin homolog-induced putative kinase 1 () (n = 4), parkin () (n = 3), or the leucine-rich repeat kinase 2 () c.6055 G to A transition (n = 3). In addition, 5 patients with more atypical disease were compound heterozygotes for the glucocerebrosidase gene () (n = 3) 1 was heterozygous for solute carrier family 2, member 1 () and another carried a novel ataxin 2 () exon 1 duplication. In most patients, the cumulative mutational burden did not appear to contribute to age at onset or progression.
CONCLUSION
In this clinical series, 15 patients (14%) carried mutations that were linked to monogenic parkinsonism. carriers were most likely to suffer an earlier cognitive demise. Nevertheless, the etiology for most patients with early onset PD remains to be determined.
背景
帕金森病(PD)的初始诊断具有挑战性,尤其是对于早发型和非典型疾病患者。帕金森综合征的遗传病因一旦确定,便可结束诊断之旅,并可为预后和治疗提供依据。本研究的目的是阐明早发型疾病(发病年龄<45岁)患者帕金森综合征的遗传病因。
方法
进行全外显子组测序、拷贝数变异分析和短串联重复分析。分析集中于先前与早发型帕金森综合征患者的帕金森综合征和肌张力障碍相关的基因。使用回归模型评估基因型-表型相关性。
结果
患者队列的特征为早发型、缓慢进展的帕金森综合征,平均发病年龄为39.2±5.0岁(n=108)。病程达10年时,平均Hoehn&Yahr分期为2.6±0.8,统一帕金森病评定量表第三部分(运动部分)平均评分为24.9±12.1(n=83),30例患者在最后一次检查时存在认知障碍(蒙特利尔认知评估评分≤26)。10例典型早发型PD患者携带纯合或复合杂合突变,分别为磷酸酶和张力蛋白同源物诱导的假定激酶1()(n=4)、帕金森蛋白()(n=3)或富含亮氨酸重复激酶2()c.6055G到A的转换(n=3)。此外,5例病情更不典型的患者为葡萄糖脑苷脂酶基因()的复合杂合子(n=3),1例为溶质载体家族2成员1()杂合子,另1例携带新的ataxin 2()外显子1重复突变。在大多数患者中,累积突变负担似乎与发病年龄或疾病进展无关。
结论
在这个临床系列中,15例患者(14%)携带与单基因帕金森综合征相关的突变。 携带者最有可能较早出现认知功能衰退。然而,大多数早发型PD患者的病因仍有待确定。
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