早发性帕金森病中Parkin和PINK1突变:对公开病例和对照进行全面筛查
Parkin and PINK1 mutations in early-onset Parkinson's disease: comprehensive screening in publicly available cases and control.
作者信息
Brooks J, Ding J, Simon-Sanchez J, Paisan-Ruiz C, Singleton A B, Scholz S W
机构信息
Laboratory of Neurogenetics, National Institute on Aging, 35 Convent Drive, 20892 Bethesda, USA.
出版信息
J Med Genet. 2009 Jun;46(6):375-81. doi: 10.1136/jmg.2008.063917. Epub 2009 Apr 6.
BACKGROUND
Mutations in parkin and PTEN-induced protein kinase (PINK1) represent the two most common causes of autosomal recessive parkinsonism. The possibility that heterozygous mutations in these genes also predispose to disease or lower the age of disease onset has been suggested, but currently there is insufficient data to verify this hypothesis conclusively.
OBJECTIVE
To study the frequency and spectrum of parkin and PINK1 gene mutations and to investigate the role of heterozygous mutations as a risk factor for early-onset Parkinson's disease (PD).
METHODS
All exons and exon-intron boundaries of PINK1 and parkin were sequenced in 250 patients with early-onset PD and 276 normal controls. Gene dosage measurements were also performed, using high-density single-nucleotide polymorphism arrays.
RESULTS
In total 41 variants were found, of which 8 have not been previously described (parkin: p.A38VfsX6, p.C166Y, p.Q171X, p.D243N, p.M458L; PINK1: p.P52L, p.T420T, p.A427E). 1.60% of patients were homozygous or compound heterozygous for pathogenic mutations. Heterozygosity for pathogenic parkin or PINK1 mutations was over-represented in patients compared with healthy controls (4.00% vs. 1.81%) but the difference was not significant (p = 0.13). The mean age at disease onset was significantly lower in patients with homozygous or compound heterozygous mutations than in patients with heterozygous mutations (mean difference 11 years, 95% CI 1.4 to 20.6, p = 0.03). There was no significant difference in the mean age at disease onset in heterozygous patients compared with patients without a mutation in parkin or PINK1 (mean difference 2 years, 95% CI -3.7 to 7.0, p = 0.54).
CONCLUSIONS
Our data support a trend towards a higher frequency of heterozygosity for pathogenic parkin or PINK1 mutations in patients compared with normal controls, but this effect was small and did not reach significance in our cohort of 250 cases and 276 controls.
背景
帕金森病蛋白(parkin)和PTEN诱导激酶(PINK1)的突变是常染色体隐性帕金森综合征最常见的两种病因。有研究表明这些基因的杂合突变也可能导致疾病或降低发病年龄,但目前尚无足够数据能最终证实这一假设。
目的
研究parkin和PINK1基因突变的频率及范围,并探讨杂合突变作为早发性帕金森病(PD)危险因素的作用。
方法
对250例早发性PD患者和276例正常对照者的PINK1和parkin所有外显子及外显子-内含子边界进行测序。同时使用高密度单核苷酸多态性阵列进行基因剂量测量。
结果
共发现41个变异,其中8个变异此前未见报道(parkin:p.A38VfsX6、p.C166Y、p.Q171X、p.D243N、p.M458L;PINK1:p.P52L、p.T420T、p.A427E)。1.60%的患者为致病突变的纯合子或复合杂合子。与健康对照相比,致病的parkin或PINK1基因突变杂合子在患者中比例过高(4.00% 对1.81%),但差异无统计学意义(p = 0.13)。纯合子或复合杂合子突变患者的平均发病年龄显著低于杂合子突变患者(平均差异11岁,95% CI 1.4至20.6,p = 0.03)。与parkin或PINK1无突变的患者相比,杂合子患者的平均发病年龄差异无统计学意义(平均差异2岁,95% CI -3.7至7.0,p = 0.54)。
结论
我们的数据支持与正常对照相比,患者中致病的parkin或PINK1基因突变杂合子频率有升高趋势,但这种影响较小,在我们250例病例和276例对照的队列中未达到统计学意义。
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