Cyclin-G-associated kinase modifies alpha-synuclein expression levels and toxicity in Parkinson's disease: results from the GenePD Study

Dumitriu, A.; Pacheco, C. D.; Wilk, J. B.; Strathearn, K. E.; Latourelle, J. C.; Goldwurm, S.; Pezzoli, G.; Rochet, J.-C.; Lindquist, S.; Myers, R. H.

Author(s)

Dumitriu, Alexandra; Pacheco, Chris D.; Wilk, Jemma B.; Strathearn, Katherine E.; Latourelle, Jeanne C.; ... Show more

DownloadLindquist_Cyclin-G.pdf (212.2Kb)

PUBLISHER_POLICY

Terms of use

Article is made available in accordance with the publisher's policy and may be subject to US copyright law. Please refer to the publisher's site for terms of use.

Metadata

Show full item record

Abstract

Although family history is a well-established risk factor for Parkinson's disease (PD), fewer than 5% of PD cases can be attributed to known genetic mutations. The etiology for the remainder of PD cases is unclear; however, neuronal accumulation of the protein α-synuclein is common to nearly all patients, implicating pathways that influence α-synuclein in PD pathogenesis. We report a genome-wide significant association (P = 3.97 × 10−8) between a polymorphism, rs1564282, in the cyclin-G-associated kinase (GAK) gene and increased PD risk, with a meta-analysis odds ratio of 1.48. This association result is based on the meta-analysis of three publicly available PD case–control genome-wide association study and genotyping from a new, independent Italian cohort. Microarray expression analysis of post-mortem frontal cortex from PD and control brains demonstrates a significant association between rs1564282 and higher α-synuclein expression, a known cause of early onset PD. Functional knockdown of GAK in cell culture causes a significant increase in toxicity when α-synuclein is over-expressed. Furthermore, knockdown of GAK in rat primary neurons expressing the A53T mutation of α-synuclein, a well-established model for PD, decreases cell viability. These observations provide evidence that GAK is associated with PD risk and suggest that GAK and α-synuclein interact in a pathway involved in PD pathogenesis. The GAK protein, a serine/threonine kinase, belongs to a family of proteins commonly targeted for drug development. This, combined with GAK's observed relationship to the levels of α-synuclein expression and toxicity, suggests that the protein is an attractive therapeutic target for the treatment of PD.

Date issued

2011-01

URI

http://hdl.handle.net/1721.1/65570

Department

move to dc.description.sponsorship; Massachusetts Institute of Technology. Department of Biology

Journal

Human Molecular Genetics

Publisher

Oxford University Press

Citation

Dumitriu, A. et al. “Cyclin-G-associated Kinase Modifies -synuclein Expression Levels and Toxicity in Parkinson’s Disease: Results from the GenePD Study.” Human Molecular Genetics 20.8 (2011) : 1478-1487.

Version: Final published version

ISSN

0964-6906

1460-2083

Collections

MIT Open Access Articles

DSpace@MIT