Analysis of the genetic variability in Parkinson's disease from Southern Spain

S Bandrés-Ciga, NE Mencacci, R Durán, FJ Barrero… - Neurobiology of …, 2016 - Elsevier
S Bandrés-Ciga, NE Mencacci, R Durán, FJ Barrero, F Escamilla-Sevilla, S Morgan, J Hehir
Neurobiology of aging, 2016Elsevier
To date, a large spectrum of genetic variants has been related to familial and sporadic
Parkinson's disease (PD) in diverse populations worldwide. However, very little is known
about the genetic landscape of PD in Southern Spain, despite its particular genetic
landscape coming from multiple historical migrations. We included 134 PD patients in this
study, of which 97 individuals were diagnosed with late-onset sporadic PD (LOPD), 28 with
early-onset sporadic PD (EOPD), and 9 with familial PD (FPD). Genetic analysis was …
Abstract
To date, a large spectrum of genetic variants has been related to familial and sporadic Parkinson's disease (PD) in diverse populations worldwide. However, very little is known about the genetic landscape of PD in Southern Spain, despite its particular genetic landscape coming from multiple historical migrations. We included 134 PD patients in this study, of which 97 individuals were diagnosed with late-onset sporadic PD (LOPD), 28 with early-onset sporadic PD (EOPD), and 9 with familial PD (FPD). Genetic analysis was performed through a next-generation sequencing panel to screen 8 PD-related genes (LRRK2, SNCA, PARKIN, PINK1, DJ-1, VPS35, GBA, and GCH1) in EOPD and FPD groups and direct Sanger sequencing of GBA exons 8–11 and LRRK2 exons 31 and 41 in the LOPD group. In the EOPD and FPD groups, we identified 11 known pathogenic mutations among 15 patients (40.5 %). GBA (E326K, N370S, D409H, L444P) mutations were identified in 7 patients (18.9 %); LRRK2 (p.R1441G and p.G2019S) in 3 patients (8.1 %); biallelic PARK2 mutations (p.N52fs, p.V56E, p.C212Y) in 4 cases (10.8%) and PINK1 homozygous p.G309D in 1 patient (2.7 %). An EOPD patient carried a single PARK2 heterozygous mutation (p.R402C), and another had a novel heterozygous mutation in VPS35 (p.R32S), both of unknown significance. Moreover, pathogenic mutations in GBA (E326K, T369M, N370S, D409H, L444P) and LRRK2 (p.R1441G and p.G2019S) were identified in 13 patients (13.4 %) and 4 patients (4.1 %), respectively, in the LOPD group. A large number of known pathogenic mutations related to PD have been identified. In particular, GBA and LRRK2 mutations appear to be considerably frequent in our population, suggesting a strong Jewish influence. Further research is needed to study the contribution of the novel found mutation p.R32S in VPS35 to the pathogenesis of PD.
Elsevier
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