4.7 Article

Chemogenetic modulation of cholinergic interneurons reveals their regulating role on the direct and indirect output pathways from the striatum

期刊

NEUROBIOLOGY OF DISEASE
卷 109, 期 -, 页码 148-162

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.nbd.2017.10.010

关键词

L-DOPA induced dyskinesias; Parkinson's disease; Animal models; Chemogenetics; DREADD; Cholinergic interneurons; AAV; Transgenic rats; Indirect pathway; Direct pathway

资金

  1. Parkinson's Disease Foundation International Research Grant [PDF-IRG-1303]
  2. Swedish Research Council [K2014-79X-22510-01-1, AR-MH-2016-01997]
  3. Swedish Parkinson Foundation
  4. Swedish Alzheimer foundation
  5. Crafoord foundation
  6. Bagadilico Linnaeus consortium
  7. Schyberg foundation
  8. Thuring foundation
  9. Kocks foundation
  10. Ake Wiberg foundation
  11. Ahlen foundation
  12. Magnus Bergvall foundation
  13. Tore Nilsson foundation
  14. Swedish Neuro foundation
  15. OE and Edla Johanssons foundation
  16. Lars Hierta foundation
  17. Bente Rexed foundation
  18. Swedish society for medical research (SSMF)

向作者/读者索取更多资源

The intricate balance between dopaminergic and cholinergic neurotransmission in the striatum has been thoroughly difficult to characterize. It was initially described as a seesaw with a competing function of dopamine versus acetylcholine. Recent technical advances however, have brought this view into question suggesting that the two systems work rather in concert with the cholinergic interneurons (ChIs) driving dopamine release. In this study, we have utilized two transgenic Cre-driver rat lines, a choline acetyl transferase ChAT-Cre transgenic rat and a novel double-transgenic tyrosine hydroxylase TH-Cre/ChAT-Cre rat to further elucidate the role of striatal ChIs in normal motor function and in Parkinson's disease. Here we show that selective and reversible activation of ChIs using chemogenetic (DREADD) receptors increases locomotor function in intact rats and potentiate the therapeutic effect of L-DOPA in the rats with lesions of the nigral dopamine system. However, the potentiation of the L-DOPA effect is accompanied by an aggravation of L-DOPA induced dyskinesias (LIDs). These LIDs appear to be driven primarily through the indirect striato-pallidal pathway since the same effect can be induced by the D2 agonist Quinpirole. Taken together, the results highlight the intricate regulation of balance between the two output pathways from the striatum orchestrated by the ChIs.

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