Genome-wide Association and Meta-analysis of Age at Onset in Parkinson Disease: Evidence from the COURAGE-PD Consortium

Grover, S.; Sreelatha, A. A. K.; Pihlstrom, L.; Domenighetti, C.; Schulte, C.; Sugier, P. -E.; Radivojkov-Blagojevic, M.; Lichtner, P.; Mohamed, O.; Portugal, B.; Landoulsi, Z.; May, P.; Bobbili, D.; Edsall, C.; Bartusch, F.; Hanussek, M.; Kruger, J.; Hernandez, D. G.; Blauwendraat, C.; Mellick, G. D.; Zimprich, A.; Pirker, W.; Tan, M.; Rogaeva, E.; Lang, A.; Koks, S.; Taba, P.; Lesage, S.; Brice, A.; Corvol, J. -C.; Chartier-Harlin, M. -C.; Mutez, E.; Brockmann, K.; Deutschlander, A. B.; Hadjigeorgiou, G. M.; Dardiotis, E.; Stefanis, L.; Simitsi, A. M.; Valente, E. M.; Petrucci, S.; Straniero, L.; Zecchinelli, A.; Pezzoli, G.; Brighina, L.; Ferrarese, C.; Annesi, G.; Quattrone, A.; Gagliardi, M.; Burbulla, L. F.; Matsuo, H.; Kawamura, Y.; Hattori, N.; Nishioka, K.; Chung, S. J.; Kim, Y. J.; Pavelka, L.; Van De Warrenburg, B. P. C.; Bloem, B. R.; Singleton, A. B.; Aasly, J.; Toft, M.; Guedes, L. C.; Ferreira, J. J.; Bardien, S.; Carr, J.; Tolosa, E.; Ezquerra, M.; Pastor, P.; Diez-Fairen, M.; Wirdefeldt, K.; Pedersen, N. L.; Ran, C.; Belin, A. C.; Puschmann, A.; Hellberg, C.; Clarke, C. E.; Morrison, K. E.; Krainc, D.; Farrer, M. J.; Kruger, R.; Elbaz, A.; Gasser, T.; Sharma, M.

doi:10.1212/WNL.0000000000200699

Background and Objectives Considerable heterogeneity exists in the literature concerning genetic determinants of the age at onset (AAO) of Parkinson disease (PD), which could be attributed to a lack of well-powered replication cohorts. The previous largest genome-wide association studies (GWAS) identified SNCA and TMEM175 loci on chromosome (Chr) 4 with a significant influence on the AAO of PD; these have not been independently replicated. This study aims to conduct a meta-analysis of GWAS of PD AAO and validate previously observed findings in worldwide populations. Methods A meta-analysis was performed on PD AAO GWAS of 30 populations of predominantly European ancestry from the Comprehensive Unbiased Risk Factor Assessment for Genetics and Environment in Parkinson's Disease (COURAGE-PD) Consortium. This was followed by combining our study with the largest publicly available European ancestry dataset compiled by the International Parkinson Disease Genomics Consortium (IPDGC). Results The COURAGE-PD Consortium included a cohort of 8,535 patients with PD (91.9%: Europeans and 9.1%: East Asians). The average AAO in the COURAGE-PD dataset was 58.9 years (SD = 11.6), with an underrepresentation of females (40.2%). The heritability estimate for AAO in COURAGE-PD was 0.083 (SE = 0.057). None of the loci reached genome-wide significance (p < 5 × 10-8). Nevertheless, the COURAGE-PD dataset confirmed the role of the previously published TMEM175 variant as a genetic determinant of the AAO of PD with Bonferroni-corrected nominal levels of significance (p < 0.025): (rs34311866: β(SE)COURAGE = 0.477(0.203), pCOURAGE = 0.0185). The subsequent meta-analysis of COURAGE-PD and IPDGC datasets (Ntotal = 25,950) led to the identification of 2 genome-wide significant association signals on Chr 4, including the previously reported SNCA locus (rs983361: β(SE)COURAGE+IPDGC = 0.720(0.122), pCOURAGE+IPDGC = 3.13 × 10-9) and a novel BST1 locus (rs4698412: β(SE)COURAGE+IPDGC = -0.526(0.096), pCOURAGE+IPDGC = 4.41 × 10-8). Discussion Our study further refines the genetic architecture of Chr 4 underlying the AAO of the PD phenotype through the identification of BST1 as a novel AAO PD locus. These findings open a new direction for the development of treatments to delay the onset of PD.