Sun Mei, Latourelle Jeanne C, Wooten G Frederick, Lew Mark F, Klein Christine, Shill Holly A, Golbe Lawrence I, Mark Margery H, Racette Brad A, Perlmutter Joel S, Parsian Abbas, Guttman Mark, Nicholson Garth, Xu Gang, Wilk Jemma B, Saint-Hilaire Marie H, DeStefano Anita L, Prakash Ranjana, Williamson Sally, Suchowersky Oksana, Labelle Nancy, Growdon John H, Singer Carlos, Watts Ray L, Goldwurm Stefano, Pezzoli Gianni, Baker Kenneth B, Pramstaller Peter P, Burn David J, Chinnery Patrick F, Sherman Scott, Vieregge Peter, Litvan Irene, Gillis Tammy, MacDonald Marcy E, Myers Richard H, Gusella James F
Molecular Neurogenetics Unit, Center for Human Genetic Research, Massachusetts General Hospital, Harvard Medical School, Boston 02114, USA.
Arch Neurol. 2006 Jun;63(6):826-32. doi: 10.1001/archneur.63.6.826.
The PARK2 gene at 6q26 encodes parkin, whose inactivation is implicated in an early-onset autosomal recessive form of Parkinson disease (PD).
To evaluate the influence of heterozygosity for parkin mutation on onset age in a sample of families with at least 2 PD-affected members.
Clinical and genetic study.
Twenty collaborative clinical sites.
Patients with familial PD collected in the GenePD study. Studied families were selected for (1) affected sibling pairs sharing 2 alleles identical by state at PARK2 (D6S305) or (2) 1 or more family members with onset age younger than 54 years, regardless of D6S305 status. At least 1 member from each of 183 families underwent comprehensive screening for deletion/insertion variants and point mutations in PARK2.
Mutations in the parkin gene were screened by means of single-stranded conformation polymorphism and sequencing in all 12 coding exons and flanking intronic sequences for point mutations and duplex quantitative polymerase chain reaction in all exons for rearrangement, duplication, and deletion.
Mutations were found in 23 families (12.6% of those screened). Among the mutation-positive families, 10 (43%) contained compound heterozygotes; 3 (13%), homozygotes; and 10 (43%), heterozygotes. The onset age in patients with parkin gene mutations ranged from 20 to 76 years. Patients with 1 parkin mutation had an 11.7-year age at onset than did patients with none (P = .04), and patients with 2 or more parkin mutations had a 13.2-year decrease in age at onset compared with patients with 1 mutation (P = .04).
These data indicate that parkin mutations are not rare in multiply affected sibships, and that heterozygous mutation carrier status in PARK2 significantly influences age at onset of PD.
位于6q26的PARK2基因编码帕金森蛋白,其失活与早发性常染色体隐性帕金森病(PD)有关。
在至少有2名PD患者的家系样本中,评估帕金森蛋白突变杂合性对发病年龄的影响。
临床和遗传学研究。
20个合作临床站点。
基因PD研究中收集的家族性PD患者。入选研究的家系需满足以下条件之一:(1)在PARK2(D6S305)位点共享2个相同状态等位基因的患病同胞对;(2)1名或多名发病年龄小于54岁的家庭成员,无论D6S305状态如何。对183个家系中的至少1名成员进行了PARK2基因缺失/插入变异和点突变的全面筛查。
通过单链构象多态性和测序对帕金森蛋白基因的所有12个编码外显子及其侧翼内含子序列进行点突变筛查,通过双链定量聚合酶链反应对外显子进行重排、重复和缺失检测。
在23个家系(占筛查家系的12.6%)中发现了突变。在突变阳性家系中,10个(43%)为复合杂合子;3个(13%)为纯合子;10个(43%)为杂合子。帕金森蛋白基因突变患者的发病年龄在20至76岁之间。有1个帕金森蛋白突变的患者发病年龄比无突变患者早11.7岁(P = 0.04),有2个或更多帕金森蛋白突变的患者发病年龄比有1个突变的患者早13.2岁(P = 0.04)。
这些数据表明,在多个患病同胞家系中,帕金森蛋白突变并不罕见,且PARK2基因杂合突变携带者状态显著影响PD的发病年龄。
