Gene-Wise Association of Variants in Four Lysosomal Storage Disorder Genes in Neuropathologically Confirmed Lewy Body Disease

Alcalay, Roy Nissim; Chan, Robin Barry; Cheng, Rong; Clark, Lorraine N.; Cortes, Etty Paola; Di Paolo, Gilbert; Fahn, Stanley; Honig, Lawrence S.; Kisselev, Sergey; Lee, Joseph H.; Liu, Xinmin; Marder, Karen; Mayeux, Richard Paul; Park, Naeun; Parmalee, Nancy; Pastores, Gregory M.; Shelanski, Michael L.; Torres, Paola A.; Vonsattel, Jean Paul

Gene-Wise Association of Variants in Four Lysosomal Storage Disorder Genes in Neuropathologically Confirmed Lewy Body Disease

Authors: Roy Nissim Alcalay
Robin Barry Chan
Rong Cheng
Lorraine N. Clark
Etty Paola Cortes
Gilbert Di Paolo
Stanley Fahn
Lawrence S. Honig
Sergey Kisselev
Joseph H. Lee
Xinmin Liu
Karen Marder
Richard Paul Mayeux
Naeun Park
Nancy Parmalee
Gregory M. Pastores
Michael L. Shelanski
Paola A. Torres
Jean Paul Vonsattel
Publication date: 1 January 2015
Publisher: 'Columbia University Libraries/Information Services'
Doi

Abstract

Objective Variants in GBA are associated with Lewy Body (LB) pathology. We investigated whether variants in other lysosomal storage disorder (LSD) genes also contribute to disease pathogenesis. Methods We performed a genetic analysis of four LSD genes including GBA, HEXA, SMPD1, and MCOLN1 in 231 brain autopsies. Brain autopsies included neuropathologically defined LBD without Alzheimer Disease (AD) changes (n = 59), AD without significant LB pathology (n = 71), Alzheimer disease and lewy body variant (ADLBV) (n = 68), and control brains without LB or AD neuropathology (n = 33). Sequencing of HEXA, SMPD1, MCOLN1 and GBA followed by ‘gene wise’ genetic association analysis was performed. To determine the functional effect, a biochemical analysis of GBA in a subset of brains was also performed. GCase activity was measured in a subset of brain samples (n = 64) that included LBD brains, with or without GBA mutations, and control brains. A lipidomic analysis was also performed in brain autopsies (n = 67) which included LBD (n = 34), ADLBV (n = 3), AD (n = 4), PD (n = 9) and control brains (n = 17), comparing GBA mutation carriers to non-carriers. Results In a ‘gene-wise’ analysis, variants in GBA, SMPD1 and MCOLN1 were significantly associated with LB pathology (p range: 0.03–4.14 x10-5). Overall, the mean levels of GCase activity were significantly lower in GBA mutation carriers compared to non-carriers (p<0.001). A significant increase and accumulation of several species for the lipid classes, ceramides and sphingolipids, was observed in LBD brains carrying GBA mutations compared to controls (p range: p<0.05-p<0.01). Interpretation Our study indicates that variants in GBA, SMPD1 and MCOLN1 are associated with LB pathology. Biochemical data comparing GBA mutation carrier to non-carriers support these findings, which have important implications for biomarker development and therapeutic strategies