The LRRK2 Variant E193K Prevents Mitochondrial Fission Upon MPP+ Treatment by Altering LRRK2 Binding to DRP1.

LRRK2 变体 E193K 通过改变 LRRK2 与 DRP1 的结合来阻止 MPP+ 处理引起的线粒体分裂

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作者：Perez Carrion Maria, Pischedda Francesca, Biosa Alice, Russo Isabella, Straniero Letizia, Civiero Laura, Guida Marianna, Gloeckner Christian J, Ticozzi Nicola, Tiloca Cinzia, Mariani Claudio, Pezzoli Gianni, Duga Stefano, Pichler Irene, Pan Lifeng, Landers John E, Greggio Elisa, Hess Michael W, Goldwurm Stefano, Piccoli Giovanni

期刊：	Frontiers in Molecular Neuroscience	影响因子：	3.800
时间：	2018	起止号：	2018 Feb 28; 11:64
doi：	10.3389/fnmol.2018.00064	研究方向：	其它

Mutations in leucine-rich repeat kinase 2 gene (LRRK2) are associated with familial and sporadic Parkinson's disease (PD). LRRK2 is a complex protein that consists of multiple domains, including 13 putative armadillo-type repeats at the N-terminus. In this study, we analyzed the functional and molecular consequences of a novel variant, E193K, identified in an Italian family. E193K substitution does not influence LRRK2 kinase activity. Instead it affects LRRK2 biochemical properties, such as phosphorylation at Ser935 and affinity for 14-3-3Îµ. Primary fibroblasts obtained from an E193K carrier demonstrated increased cellular toxicity and abnormal mitochondrial fission upon 1-methyl-4-phenylpyridinium treatment. We found that E193K alters LRRK2 binding to DRP1, a crucial mediator of mitochondrial fission. Our data support a role for LRRK2 as a scaffolding protein influencing mitochondrial fission.

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