Frontiers in Cellular Neuroscience (Apr 2021)

Striatal Dopamine Transporter Function Is Facilitated by Converging Biology of α-Synuclein and Cholesterol

  • Sarah Threlfell,
  • Sarah Threlfell,
  • Amir Saeid Mohammadi,
  • Brent J. Ryan,
  • Brent J. Ryan,
  • Natalie Connor-Robson,
  • Natalie Connor-Robson,
  • Nicola J. Platt,
  • Rishi Anand,
  • Florence Serres,
  • Trevor Sharp,
  • Nora Bengoa-Vergniory,
  • Nora Bengoa-Vergniory,
  • Richard Wade-Martins,
  • Richard Wade-Martins,
  • Andrew Ewing,
  • Stephanie J. Cragg,
  • Stephanie J. Cragg,
  • Katherine R. Brimblecombe,
  • Katherine R. Brimblecombe

DOI
https://doi.org/10.3389/fncel.2021.658244
Journal volume & issue
Vol. 15

Abstract

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Striatal dopamine transporters (DAT) powerfully regulate dopamine signaling, and can contribute risk to degeneration in Parkinson’s disease (PD). DATs can interact with the neuronal protein α-synuclein, which is associated with the etiology and molecular pathology of idiopathic and familial PD. Here, we tested whether DAT function in governing dopamine (DA) uptake and release is modified in a human-α-synuclein-overexpressing (SNCA-OVX) transgenic mouse model of early PD. Using fast-scan cyclic voltammetry (FCV) in ex vivo acute striatal slices to detect DA release, and biochemical assays, we show that several aspects of DAT function are promoted in SNCA-OVX mice. Compared to background control α-synuclein-null mice (Snca-null), the SNCA-OVX mice have elevated DA uptake rates, and more pronounced effects of DAT inhibitors on evoked extracellular DA concentrations ([DA]o) and on short-term plasticity (STP) in DA release, indicating DATs play a greater role in limiting DA release and in driving STP. We found that DAT membrane levels and radioligand binding sites correlated with α-synuclein level. Furthermore, DAT function in Snca-null and SNCA-OVX mice could also be promoted by applying cholesterol, and using Tof-SIMS we found genotype-differences in striatal lipids, with lower striatal cholesterol in SNCA-OVX mice. An inhibitor of cholesterol efflux transporter ABCA1 or a cholesterol chelator in SNCA-OVX mice reduced the effects of DAT-inhibitors on evoked [DA]o. Together these data indicate that human α-synuclein in a mouse model of PD promotes striatal DAT function, in a manner supported by extracellular cholesterol, suggesting converging biology of α-synuclein and cholesterol that regulates DAT function and could impact DA function and PD pathophysiology.

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