Common genetic variants associated with Parkinson's disease display widespread signature of epigenetic plasticity

Parkinson disease (PD) is characterized by a pivotal progressive loss of substantia nigra dopaminergic neurons and aggregation of alpha-synuclein protein encoded by the SNCA gene. Genome-wide association studies identified almost 100 sequence variants linked to PD in SNCA. However, the consequences of this genetic variability are rather unclear. Herein, our analysis on selective single nucleotide polymorphisms (SNPs) which are highly associated with the PD susceptibility revealed that several SNP sites attribute to the nucleosomes and overlay with bivalent regions poised to adopt either active or repressed chromatin states. We also identified large number of transcription factor (TF) binding sites associated with these variants. In addition, we located two docking sites in the intron-1 methylation prone region of SNCA which are required for the putative interactions with DNMT1. Taken together, our analysis reflects an additional layer of epigenomic contribution for the regulation of the SNCA gene in PD.

Common genetic variants associated with Parkinson's disease display widespread signature of epigenetic plasticity

Associations of genetic and infectious risk factors with coronary heart disease

Using population-specific add-on polymorphisms to improve genotype imputation in underrepresented populations

The interplay between human genetic variation, chronic inflammation and persistent infection: relevance for cardiovascular morbidity

Associations of genetic and infectious risk factors with coronary heart disease

Using population-specific add-on polymorphisms to improve genotype imputation in underrepresented populations

The interplay between human genetic variation, chronic inflammation and persistent infection: relevance for cardiovascular morbidity