4.8 Article

Mechanisms of amphetamine action illuminated through optical monitoring of dopamine synaptic vesicles in Drosophila brain

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NATURE COMMUNICATIONS
卷 7, 期 -, 页码 -

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NATURE PUBLISHING GROUP
DOI: 10.1038/ncomms10652

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资金

  1. Leon Levy Foundation
  2. NARSAD Young Investigator Award [K05 DA022413, P01 DA12408]
  3. Lieber Center for Schizophrenia Research and Treatment award [R01 DA007418, PO1 DA0 10154]
  4. JPB and Parkinson's Disease Foundations
  5. G. Harold & Leila Y. Mathers Charitable Foundation [NS075572, AG08702]
  6. Dana Foundation
  7. Gatsby Initiative in Brain Circuitry
  8. New York Presbyterian Seizure Disorders Fund [R01 MH076900, R01 ES015747, P01 ES016732]
  9. Brain and behaviour Research Foundation
  10. Brain Research Institute
  11. UCLA Molecular Toxicology Program
  12. Intramural Research Program of NIDA
  13. [K08 DA031241]
  14. [R01 MH086545]
  15. [T32 ES015457]
  16. [GM07185]
  17. [R01 NS075222]

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Amphetamines elevate extracellular dopamine, but the underlying mechanisms remain uncertain. Here we show in rodents that acute pharmacological inhibition of the vesicular monoamine transporter (VMAT) blocks amphetamine-induced locomotion and self-administration without impacting cocaine-induced behaviours. To study VMAT's role in mediating amphetamine action in dopamine neurons, we have used novel genetic, pharmacological and optical approaches in Drosophila melanogaster. In an ex vivo whole-brain preparation, fluorescent reporters of vesicular cargo and of vesicular pH reveal that amphetamine redistributes vesicle contents and diminishes the vesicle pH-gradient responsible for dopamine uptake and retention. This amphetamine-induced deacidification requires VMAT function and results from net H+ antiport by VMAT out of the vesicle lumen coupled to inward amphetamine transport. Amphetamine-induced vesicle deacidification also requires functional dopamine transporter (DAT) at the plasma membrane. Thus, we find that at pharmacologically relevant concentrations, amphetamines must be actively transported by DAT and VMAT in tandem to produce psychostimulant effects.

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