Litcius/Paper detail

LRRK2 and Lipid Pathways: Implications for Parkinson’s Disease

Jasmin Galper, Woojin S. Kim, Nicolas Dzamko

2022Biomolecules24 citationsDOIOpen Access PDF

Abstract

gene, encoding leucine-rich repeat kinase 2, are a common risk factor for Parkinson's disease. How LRRK2 alterations lead to cell pathology is an area of ongoing investigation, however, multiple lines of evidence suggest a role for LRRK2 in lipid pathways. It is increasingly recognized that in addition to being energy reservoirs and structural entities, some lipids, including neural lipids, participate in signaling cascades. Early investigations revealed that LRRK2 localized to membranous and vesicular structures, suggesting an interaction of LRRK2 and lipids or lipid-associated proteins. LRRK2 substrates from the Rab GTPase family play a critical role in vesicle trafficking, lipid metabolism and lipid storage, all processes which rely on lipid dynamics. In addition, LRRK2 is associated with the phosphorylation and activity of enzymes that catabolize plasma membrane and lysosomal lipids. Furthermore, LRRK2 knockout studies have revealed that blood, brain and urine exhibit lipid level changes, including alterations to sterols, sphingolipids and phospholipids, respectively. In human LRRK2 mutation carriers, changes to sterols, sphingolipids, phospholipids, fatty acyls and glycerolipids are reported in multiple tissues. This review summarizes the evidence regarding associations between LRRK2 and lipids, and the functional consequences of LRRK2-associated lipid changes are discussed.

Topics & Concepts

LRRK2SphingolipidRabLipid metabolismGTPaseCell biologyBiologyKinaseLipid microdomainBiochemistryLipid dropletLipid raftLipidomicsSignal transductionMutationGeneMembraneParkinson's Disease Mechanisms and TreatmentsCellular transport and secretionLysosomal Storage Disorders Research