LRRK1-LRRK2 异二聚化:对 LRRK2 相关帕金森病的影响。
Heterodimerization of Lrrk1-Lrrk2: Implications for LRRK2-associated Parkinson disease.
机构信息
Division of Neurogenetics, Department of Neuroscience, Mayo Clinic, 4500 San Pablo Road, Jacksonville, FL 32224, USA.
出版信息
Mech Ageing Dev. 2010 Mar;131(3):210-4. doi: 10.1016/j.mad.2010.01.009. Epub 2010 Feb 6.
Abstract
LRRK2 mutations are recognized as the most frequent genetic cause of both familial and sporadic parkinsonism identified to date. A remarkable feature of this form of parkinsonism is the variable penetrance of symptom manifestation resulting in a wide range of age-at-onset in patients. Herein we use a functional approach to identify the Lrrk1 protein as a potential disease modifier demonstrating an interaction and heterodimer formation with Lrrk2. In addition, evaluation of LRRK1 variants in our large Lrrk2 p.G2019S-parkinsonism series from a Tunisian (n=145) identified a missense mutation (p.L416M) resulting in an average 6.2 years younger age at disease onset. In conclusion we show that the interaction of Lrrk1-Lrrk2 can form protein dimers and this interaction may influence the age of symptomatic manifestation in Lrrk2-parkinsonism patients.
摘要
LRRK2 突变被认为是迄今为止发现的家族性和散发性帕金森病最常见的遗传原因。这种形式的帕金森病的一个显著特征是症状表现的可变外显率,导致患者的发病年龄范围很广。在此,我们采用功能方法鉴定 Lrrk1 蛋白作为一种潜在的疾病修饰因子,证明其与 Lrrk2 相互作用并形成异二聚体。此外,在我们来自突尼斯的大型 Lrrk2 p.G2019S-帕金森病系列(n=145)中对 LRRK1 变体的评估中,发现了一个错义突变(p.L416M),导致疾病发病年龄平均年轻 6.2 岁。总之,我们表明 Lrrk1-Lrrk2 的相互作用可以形成蛋白质二聚体,这种相互作用可能会影响 Lrrk2-帕金森病患者的症状表现年龄。
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