Four novel rare mutations of PLA2G6 in Chinese population with Parkinson's disease

Abstract Background Mutations in the phospholipase A2 Group 6 (PLA2G6) gene have been identified in autosomal recessive neurodegenerative diseases classified as infantile neuroaxonal dystrophy and neurodegeneration with brain iron accumulation. Recently, PLA2G6 was also reported as the causative gen...

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Bibliographic Details
Published in:Parkinsonism & related disorders 2013-01, Vol.19 (1), p.21-26
Main Authors: Gui, Ya-Xing, Xu, Zhong-Ping, Wen-Lv, Liu, Hong-mei, Zhao, Jin-Jia, Hu, Xing-Yue
Format: Article
Language:English
Subjects:
Age
Age of Onset
Aged
Amino Acid Sequence
Asian Continental Ancestry Group - genetics
Basal ganglia
Brain
Central nervous system diseases
Chinese populations
Dystrophy
Female
Genetic Predisposition to Disease - genetics
Group VI Phospholipases A2 - genetics
Humans
Iron
Male
Middle Aged
Molecular Sequence Data
Movement disorders
Mutation
Mutation - genetics
Mutations
Neurodegenerative diseases
Neurology
Parkinson Disease - genetics
Parkinson's disease
Parkinson's diseases
Phospholipase
Phospholipase A2
Phospholipases A2 - genetics
PLA2G6
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Summary:Abstract Background Mutations in the phospholipase A2 Group 6 (PLA2G6) gene have been identified in autosomal recessive neurodegenerative diseases classified as infantile neuroaxonal dystrophy and neurodegeneration with brain iron accumulation. Recently, PLA2G6 was also reported as the causative gene for early-onset PARK14-linked dystonia-parkinsonism. Methods/results To address whether PLA2G6 mutations are also an important cause of PD, we screened sequence variants of PLA2G6 in 250 PD patients and 550 controls in a Chinese Han populations. We identified four sequence changes: a coding synonymous c.1959T>A transition of exon13 in one patient, two missense mutations c.1966C>G in exon13 and c.2077C>G in exon14 in two different patients, which caused two amino acids change Leu656Val and Leu693Val respectively. We also found a frame-shift mutation P.His597fx69 in exon 12 in one patient. These four rare variants were not represented in 550 control individuals. Furthermore, we found that WT PLA2G6 enzyme hydrolyzed phospholipids while mutant PLA2G6 with P.His597fx69 frame-shift caused loss of enzyme activity, exhibiting less than 6% of the specific activity in phospholipase assays compared to that of WT PLA2G6. Mutant PLA2G6 with Leu656Val and Leu693Val decreased their activity by 45% and 35% in phospholipase assay respectively. Conclusions We identified four rare PLA2G6 mutations in 250 PD patients, enlarging the spectrum of PLA2G6 mutations in PD. Although PLA2G6 mutations account for only a small fraction of PD patients in Chinese populations, these mutations impair catalytic activity of their phospholipids-hydrolyzing function. These results indicate that PLA2G6 mutations maybe PD-causing in Chinese Han populations.
ISSN:1353-8020
1873-5126
DOI:10.1016/j.parkreldis.2012.07.016