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Antiseizure and neuroprotective effects of delayed treatment with midazolam in a rodent model of organophosphate exposure.

Jay SpampanatoWendy PouliotSteven L BealerBonnie RoachFrancis Edward Dudek
Published in: Epilepsia (2019)
In conclusion, MDZ significantly reduced DFP-induced SE intensity when treatment was delayed 30, 60, and even up to 120 minutes; however, this reduction in seizure intensity had no detectable effect on neuronal death at each individual delay time. These data show that although MDZ suppressed seizures, additional neuroprotective therapies are needed to mitigate the effects of OP exposure.
Keyphrases
  • cerebral ischemia
  • high intensity
  • machine learning
  • diabetic rats
  • blood brain barrier
  • replacement therapy