Publication | Open Access
Pharmacological study of TA-0910, a new thyrotropin-releasing hormone(TRH) analog. (IV). Effects on experimental memory impairment in mice and rats.
21
Citations
41
References
1991
Year
NeuropsychologyInhibitory ProcessPsychopharmacologyDelayed Alternation TaskSocial SciencesMolecular PharmacologyPharmacological StudyNeuroendocrine MechanismMemoryNew Trh AnalogPsychiatryBehavioral NeuroscienceEndocrine MechanismNeuropharmacologyExperimental Memory ImpairmentDopamineEndocrinologyPharmacologyExperimental Analysis Of BehaviorNeurophysiologyPhysiologyNew Thyrotropin-releasing HormoneNeuroscienceThyroid HormoneMedicineAlternation Task
The effects of a new TRH analog, TA-0910, orally administered, on experimental memory impairments for the one-trial passive avoidance response in anoxic mice (light-dark box), active avoidance response in basal forebrain (BF)-lesioned rats (shuttle box), and delayed alternation task in scopolamine-treated rats (T-maze) were studied. In mice, TA-0910 (3-30 mg) administered 60 min before the retention trial dose-dependently prolonged the passive avoidance response latency reduced by CO2-exposure that was given immediately after the acquisition trial, but not when it was given 60 min before the acquisition or just after the anoxic treatment. In rats, TA-0910 (0.3-3 mg/kg) administered 40-60 min before the test trial, dose-dependently prevented the reduction in mean avoidance rate caused by BF-lesioning and elevated the scopolamine (0.1 mg/kg, i.p.)-induced reduction in percent correct choice level in the alternation task. TRH (30-300 mg/kg), on the other hand, produced no improvements in any of the above tests. These results suggest that TA-0910 improves impaired memory by correcting the retrieval process of memory.
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