R-Modafinil exerts weak effects on spatial memory acquisition and dentate gyrus synaptic plasticity

نویسندگان

  • Bharanidharan Shanmugasundaram
  • Yogesh D Aher
  • Jana Aradska
  • Marija Ilic
  • Daniel Daba Feyissa
  • Predrag Kalaba
  • Nilima Y Aher
  • Vladimir Dragacevic
  • Babak Saber Marouf
  • Thierry Langer
  • Harald H Sitte
  • Harald Hoeger
  • Gert Lubec
  • Volker Korz
چکیده

Modafinil is a wake promoting drug approved for clinical use and also has cognitive enhancing properties. Its enantiomer R-Modafinil (R-MO) is not well studied in regard to cognitive enhancing properties. Hence we studied its effect in a spatial memory paradigm and its possible effects on dentate gyrus long-term potentiation (DG-LTP). Clinically relevant doses of R-MO, vehicle dimethyl sulfoxide (DMSO) or saline were administered for three days during the hole-board test and in in vivo DG-LTP. Synaptic levels of dopamine receptors D1R, D2R, dopamine transporter (DAT), and its phosphorylated form (ph-DAT) in DG tissue 4 h after LTP induction were quantified by western blot analysis. Monoamine reuptake and release assays were performed by using transfected HEK-293 cells. Possible neurotoxic side effects on general behaviour were also studied. R-MO at both doses significantly enhanced spatial reference memory during the last training session and during memory retrieval compared to DMSO vehicle but not when compared to saline treated rats. Similarly, R-MO rescues DG-LTP from impairing effects of DMSO. DMSO reduced memory performance and LTP magnitude when compared to saline treated groups. The synaptic DR1 levels in R-MO groups were significantly decreased compared to DMSO group but were comparable with saline treated animals. We found no effect of R-MO in neurotoxicity tests. Thus, our results support the notion that LTP-like synaptic plasticity processes could be one of the factors contributing to the cognitive enhancing effects of spatial memory traces. D1R may play an important regulatory role in these processes.

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عنوان ژورنال:

دوره 12  شماره 

صفحات  -

تاریخ انتشار 2017