TY - JOUR
T1 - Evaluation of acute bis(7)-tacrine treatment on behavioral functions in 17-day-old and 30-day-old mice, with attention to drug toxicity
AU - Pan, S. Y.
AU - YU, Zhiling
AU - Dong, H.
AU - Lee, N. T.K.
AU - Wang, H.
AU - FONG, David W F
AU - Han, Y. F.
AU - Ko, K. M.
N1 - Funding Information:
This work was supported by grants from the Research Grants Council, Hong Kong (HKUST 9441/06M) and Faculty Research Grant of HKBU, FRG/05-06/II-63.
PY - 2007/4
Y1 - 2007/4
N2 - Bis(7)-tacrine was evaluated for efficacy on memory retention in mice 17 days of age and 30 days of age. The tests used were a passive-avoidance response test and a measure of spontaneous motor activity. Also, possible drug-induced hepatotoxicity and acute drug toxicity were evaluated. Behavioral studies were performed using a step-through task and an open-field test with a 24-h interval between training and evaluation tests. Bis(7)-tacrine (0.06-20 μmol/kg) was subcutaneously injected 30 min prior to the first session of both test types. During the training session of the step-through task, bis(7)-tacrine treatment reduced (by 46%, P < 0.01) the number of avoidable electric shocks (footshocks) only at a high dose of 20 μmol/kg in mice 17 days of age, but dose-dependently decreased the number of footshocks (10-56%, P < 0.001) in mice 30 days of age. Bis(7)-tacrine treatment at all doses tested did not produce any detectable changes in retention latency in mice 17 days of age, but the drug significantly prolonged retention latency at low doses (1.25 and 2.50 μmol/kg), and not high doses (5-20 μmol/kg), in mice 30 days of age. In the open-field test, bis(7)-tacrine decreased spontaneous motor activity in the acquisition session only at a high dose of 20 μmol/kg in mice 17 days of age and 30 days of age (by 28 and 45%, respectively), but did not affect spontaneous motor activity in the recall session. Bis(7)-tacrine treatment at a dose of 20 μmol/kg produced a more potent hepatotoxic effect in mice 30 days of age than in mice 17 days of age, (P < 0.05), and the drug caused acute toxicity with comparable potencies in mice of both age groups. In conclusion, mice 30 days of age seemed to be more sensitive than mice 17 days of age to bis(7)-tacrine-induced cognitive function enhancement and hepatotoxicity. Bis(7)-tacrine appears to be more potent and more selective as a cognitive function-enhancing agent than tacrine.
AB - Bis(7)-tacrine was evaluated for efficacy on memory retention in mice 17 days of age and 30 days of age. The tests used were a passive-avoidance response test and a measure of spontaneous motor activity. Also, possible drug-induced hepatotoxicity and acute drug toxicity were evaluated. Behavioral studies were performed using a step-through task and an open-field test with a 24-h interval between training and evaluation tests. Bis(7)-tacrine (0.06-20 μmol/kg) was subcutaneously injected 30 min prior to the first session of both test types. During the training session of the step-through task, bis(7)-tacrine treatment reduced (by 46%, P < 0.01) the number of avoidable electric shocks (footshocks) only at a high dose of 20 μmol/kg in mice 17 days of age, but dose-dependently decreased the number of footshocks (10-56%, P < 0.001) in mice 30 days of age. Bis(7)-tacrine treatment at all doses tested did not produce any detectable changes in retention latency in mice 17 days of age, but the drug significantly prolonged retention latency at low doses (1.25 and 2.50 μmol/kg), and not high doses (5-20 μmol/kg), in mice 30 days of age. In the open-field test, bis(7)-tacrine decreased spontaneous motor activity in the acquisition session only at a high dose of 20 μmol/kg in mice 17 days of age and 30 days of age (by 28 and 45%, respectively), but did not affect spontaneous motor activity in the recall session. Bis(7)-tacrine treatment at a dose of 20 μmol/kg produced a more potent hepatotoxic effect in mice 30 days of age than in mice 17 days of age, (P < 0.05), and the drug caused acute toxicity with comparable potencies in mice of both age groups. In conclusion, mice 30 days of age seemed to be more sensitive than mice 17 days of age to bis(7)-tacrine-induced cognitive function enhancement and hepatotoxicity. Bis(7)-tacrine appears to be more potent and more selective as a cognitive function-enhancing agent than tacrine.
KW - Acute toxicity
KW - Bis(7)-tacrine
KW - Hepatotoxicity
KW - Open-field memory
KW - Passive-avoidance response
KW - Spontaneous motor activity
UR - http://www.scopus.com/inward/record.url?scp=34249718973&partnerID=8YFLogxK
U2 - 10.1016/j.pbb.2007.03.006
DO - 10.1016/j.pbb.2007.03.006
M3 - Journal article
C2 - 17449090
AN - SCOPUS:34249718973
SN - 0091-3057
VL - 86
SP - 778
EP - 783
JO - Pharmacology Biochemistry and Behavior
JF - Pharmacology Biochemistry and Behavior
IS - 4
ER -