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MCI-225对基底前脑损伤大鼠记忆和葡萄糖利用的影响。

Effects of MCI-225 on memory and glucose utilization in basal forebrain-lesioned rats.

作者信息

Eguchi J, Iwai K, Yuasa T, Egawa M, Komatsu T, Saito K

机构信息

Pharmaceuticals Laboratory I, Yokohama Research Center, Mitsubishi Chemical Corporation, Japan.

出版信息

Pharmacol Biochem Behav. 1995 Aug;51(4):935-9. doi: 10.1016/0091-3057(95)00087-d.

Abstract

The effects of MCI-225 on amnesia, the cerebral glucose metabolism, and choline acetyltransferase (ChAT) activity in basal forebrain (BF)-lesioned rats were studied in comparison with those of tacrine. Bilateral BF lesions with ibotenic acid impaired the performance in passive avoidance (PA) tasks. Single administration of MCI-225 (10 mg/kg, PO) after a 2-week postoperative recovery period, increased the escape latencies in the PA task, but was not statistically significant. Repeated administration of MCI-225 (0.3 and 1 mg/kg, PO for 6 days) significantly reversed the PA failure. The BF-lesioned rat exhibited a marked decrease in the local cerebral glucose utilization (LCGU) in the frontal cortex, parietal cortex, and caudate-putamen. MCI-225 (1 mg/kg, PO for 5 days) significantly ameliorated the reduction of the LCGU in the parietal cortex. MCI-225 did not change the decrease in the cortical ChAT activity induced by the BF lesion. Repeated administration of tacrine reversed the PA failure (0.3 mg/kg, PO) but failed to prevent the decrement in the LCGU and the ChAT activity. These results suggest that MCI-225 could be effective in the treatment of senile dementia of the Alzheimer type, which is accompanied with both deficit in the BF-cortex cholinergic neuron and cerebral glucose hypometabolism.

摘要

研究了MCI - 225对基底前脑(BF)损伤大鼠的失忆、脑葡萄糖代谢及胆碱乙酰转移酶(ChAT)活性的影响,并与他克林进行了比较。用鹅膏蕈氨酸造成双侧BF损伤会损害被动回避(PA)任务的表现。术后恢复2周后单次给予MCI - 225(10 mg/kg,口服),可增加PA任务中的逃避潜伏期,但无统计学意义。重复给予MCI - 225(0.3和1 mg/kg,口服,共6天)可显著逆转PA失败。BF损伤大鼠额叶皮质、顶叶皮质和尾状核 - 壳核的局部脑葡萄糖利用(LCGU)显著降低。MCI - 225(1 mg/kg,口服,共5天)可显著改善顶叶皮质LCGU的降低。MCI - 225并未改变BF损伤所致的皮质ChAT活性降低。重复给予他克林可逆转PA失败(0.3 mg/kg,口服),但未能阻止LCGU和ChAT活性的降低。这些结果表明,MCI - 225可能对伴有BF - 皮质胆碱能神经元缺陷和脑葡萄糖代谢减退的阿尔茨海默型老年性痴呆有效。

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