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G2385R and I2020T Mutations Increase LRRK2 GTPase Activityopen access

Authors
Ho, Dong HwanJang, JihoonJoe, Eun-HyeSon, IlhongSeo, HyemyungSeol, Wongi
Issue Date
May-2016
Publisher
Hindawi Publishing Corporation
Keywords
DISEASE-ASSOCIATED MUTATIONS; PARKINSONS-DISEASE; KINASE-ACTIVITY; RISK-FACTOR; VARIANT; DOMAIN; GENE; LOCALIZATION; POPULATION; GLY2385ARG
Citation
BioMed Research International, v.2016, pp.1 - 9
Indexed
SCIE
SCOPUS
Journal Title
BioMed Research International
Volume
2016
Start Page
1
End Page
9
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/16112
DOI
10.1155/2016/7917128
ISSN
2314-6133
Abstract
The LRRK2 mutation is a major causal mutation in familial Parkinson's disease. Although LRRK2 contains functional GTPase and kinase domains and their activities are altered by pathogenic mutations, most studies focused on LRRK2 kinase activity because the most prevalent mutant, G2019S, enhances kinase activity. However, the G2019S mutation is extremely rare in the Asian population. Instead, the G2385R mutation was reported as a major risk factor in the Asian population. Similar to other LRRK2 studies, G2385R studies have also focused on kinase activity. Here, we investigated GTPase activities of G2385R with other LRRK2 mutants, such as G2019S, R1441C, and I2020T, as well as wild type (WT). Our results suggest that both I2020T and G2385R contain GTPase activities stronger than that of WT. A kinase assay using the commercial recombinant proteins showed that I2020T harbored stronger activity, whereas G2385R had weaker activity than that of WT, as reported previously. This is the first report of LRRK2 I2020T and G2385R GTPase activities and shows that most of the LRRK2 mutations that are pathogenic or a risk factor altered either kinase or GTPase activity, suggesting that their physiological consequences are caused by altered enzyme activities.
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