Abstract
IntroductionBoth recessive and dominant genetic forms of Parkinson’s disease have been described. The aim of this study was to assess the contribution of several genes to the pathophysiology of early onset Parkinson’s disease in a cohort from central Spain.Methods/patientsWe analyzed a cohort of 117 unrelated patients with early onset Parkinson’s disease using a pipeline, based on a combination of a next-generation sequencing panel of 17 genes previously related with Parkinson’s disease and other Parkinsonisms and CNV screening.ResultsTwenty-six patients (22.22%) carried likely pathogenic variants in PARK2, LRRK2, PINK1, or GBA. The gene most frequently mutated was PARK2, and p.Asn52Metfs*29 was the most common variation in this gene. Pathogenic variants were not observed in genes SNCA, FBXO7, PARK7, HTRA2, DNAJC6, PLA2G6, and UCHL1. Co-occurrence of pathogenic variants involving two genes was observed in ATP13A2 and PARK2 genes, as well as LRRK2 and GIGYF2 genes.ConclusionsOur results contribute to the understanding of the genetic architecture associated with early onset Parkinson’s disease, showing both PARK2 and LRRK2 play an important role in Spanish Parkinson’s disease patients. Rare variants in ATP13A2 and GIGYF2 may contribute to PD risk. However, a large proportion of genetic components remains unknown. This study might contribute to genetic diagnosis and counseling for families with early onset Parkinson’s disease.
Highlights
Both recessive and dominant genetic forms of Parkinson’s disease have been described
Pathogenic variants were not observed in genes SNCA, F-Box Protein 7 (FBXO7), PARK7, HTRA2, DNAJC6, PLA2G6, and UCHL1
Co-occurrence of pathogenic variants involving two genes was observed in ATPase Cation Transporting 13A2 (ATP13A2) and PARK2 genes, as well as Leucine-rich repeat kinase 2 (LRRK2) and GIGYF2 genes
Summary
The aim of this study was to assess the contribution of several genes to the pathophysiology of early onset Parkinson’s disease in a cohort from central Spain. Since genetic background has a higher impact on PD with early disease onset, the aim of this study was to assess the contribution of seven genes previously related to PD, and unconfirmed genes, to the pathophysiology of the EOPD in a cohort of patients from central Spain
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