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. 2018 May 18;9:451. doi: 10.3389/fphar.2018.00451

Table 1.

Mice examined in the present experiments.

Mouse number/total stimuli applied to achieve extended kindling SRS events/monitoring times AEDs tested in each mouse
Initial# (h) Later$ (h)
#1, 120 7/48 4/24 PHE25mg/kg
#2, 140 13/72 16/144 PHE25mg/kg
#3, 140 22/48 12/48 PHE25mg/kg, LEV100mg/kg
#4, 100 9/48 17/72 PHE25mg/kg, LEV100mg/kg
#5, 100 10/48 5/40 PHE25mg/kg, LEV100mg/kg
#6, 100 11/66 6/24 PHE25mg/kg, LEV100mg/kg
#7, 140 23/72 26/93 LOZ1.5mg/kg, LEV100, 400mg/kg
#8, 120 20/72 20/72 LOZ1.5mg/kg, LEV100, 400mg/kg
#9, 120 17/72 10/24 LOZ1.5mg/kg, LEV400mg
#10, 120 9/48 17/72 LOZ1.5mg/kg, LEV400mg
#11, 120 7/48 4/24 LOZ1.5mg/kg, LEV400mg
#12, 120 13/72 16/144 LOZ1.5mg/kg, LEV400mg
Mouse Number/totalandlings Applied
#1-#8, 120 0/48 h

PHE, phenytoin; LOZ, lorazepam; LEV, levetiracetam;

# and $

individual mice were monitored initially within 3 days after termination of kindling stimulation; then, monitored 8–11 weeks later. Control mice were monitored after 120 handling manipulations.