| Literature DB >> 29705185 |
Hua Wang1, Anzari Atik2, Tessandra Stewart2, Carmen Ginghina2, Patrick Aro2, Kathleen F Kerr3, John Seibyl4, Danna Jennings4, Poul Henning Jensen5, Kenneth Marek4, Min Shi2, Jing Zhang6.
Abstract
Plasma total and nervous system derived exosomal (NDE) α-synuclein have been determined as potential biomarkers of Parkinson's disease (PD). To explore the utility of plasma α-synuclein in the prodromal phase of PD, plasma total and NDE α-synuclein were evaluated in baseline and 2-year follow-up samples from 256 individuals recruited as part of the Parkinson's Associated Risk Syndrome (PARS) study. The results demonstrated that baseline and longitudinal increases in total α-synuclein predicted progression of cognitive decline in hyposmic individuals with dopamine transporter (DAT) binding reduction. On the other hand, a longitudinal decrease in NDE α-synuclein predicted worsening cognitive scores in hyposmic individuals with DAT binding reduction. Finally, in individuals with faster DAT progression, decreasing NDE/total α-synuclein ratio was associated with a larger reduction in DAT from baseline to follow-up. These results suggest that, though underlying mechanisms remain to be defined, alterations in plasma total and NDE α-synuclein concentrations are likely associated with PD progression, especially in the aspect of cognitive impairment, at early stages of the disease.Entities:
Keywords: Parkinson's; Plasma; Prodromal; Risk; α-Synuclein
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Year: 2018 PMID: 29705185 PMCID: PMC6294306 DOI: 10.1016/j.nbd.2018.04.015
Source DB: PubMed Journal: Neurobiol Dis ISSN: 0969-9961 Impact factor: 5.996