TY - JOUR
T1 - Postictal behavioral arrest in the rat
T2 - "catalepsy" or "catatonia"?
AU - Myslobodsky, Michael S.
AU - Mintz, Matti
PY - 1981/5/18
Y1 - 1981/5/18
N2 - A period of immobility following chemically (picrotoxin, metrazol) or electrically-activated (maximal electroshock) convulsions was demonstrated to possess features of neuroleptic-type catalepsy. During postictal immobility rats had vivid righting and corneal reflexes and responded t to the tail-oinch. Like haloperidol-pretreated animals they were able to remain on the vertical grid or horizontal bar for 15-60 sec or longer. Ten-fifteen minutes after seizure when catalepsy was minimal or not detectable, animals became totally unresponsive to pressure applied to the tail ("delayed analgesia"). Systematically administered haloperidol (0.25-2 mg/kg) did not affect postictal catalepsy while naloxone (5-10 mg/kg) and apomorphine (10 mg/kg) reduced the duration of the immobility period. Unlike naloxone, apomorphine diminished the intensity of cataleptic behavior. Higher doses of naloxone (20-70 mg/kg) when injected during the postictal period induced violent convulsions. None of the two drugs antagonized delayed analgesia. Daily administration of electroshock caused a build up of postictal rigidity and analgesia, coexisting with symptoms of catalepsy. Naloxone antagonised rigidity but failed to interfere with catalepsy and analgesia.
AB - A period of immobility following chemically (picrotoxin, metrazol) or electrically-activated (maximal electroshock) convulsions was demonstrated to possess features of neuroleptic-type catalepsy. During postictal immobility rats had vivid righting and corneal reflexes and responded t to the tail-oinch. Like haloperidol-pretreated animals they were able to remain on the vertical grid or horizontal bar for 15-60 sec or longer. Ten-fifteen minutes after seizure when catalepsy was minimal or not detectable, animals became totally unresponsive to pressure applied to the tail ("delayed analgesia"). Systematically administered haloperidol (0.25-2 mg/kg) did not affect postictal catalepsy while naloxone (5-10 mg/kg) and apomorphine (10 mg/kg) reduced the duration of the immobility period. Unlike naloxone, apomorphine diminished the intensity of cataleptic behavior. Higher doses of naloxone (20-70 mg/kg) when injected during the postictal period induced violent convulsions. None of the two drugs antagonized delayed analgesia. Daily administration of electroshock caused a build up of postictal rigidity and analgesia, coexisting with symptoms of catalepsy. Naloxone antagonised rigidity but failed to interfere with catalepsy and analgesia.
UR - http://www.scopus.com/inward/record.url?scp=0019420074&partnerID=8YFLogxK
U2 - 10.1016/0024-3205(81)90581-6
DO - 10.1016/0024-3205(81)90581-6
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AN - SCOPUS:0019420074
SN - 0024-3205
VL - 28
SP - 2287
EP - 2293
JO - Life Sciences
JF - Life Sciences
IS - 20
ER -